Microginin producing proteins and nucleic acids encoding a microginin gene cluster as well as methods for creating novel microginins

ABSTRACT

The invention provides for nucleic acid molecules enabling the synthesis of microginin and microginin analogues. The invention also provides for methods for identifying microginins as well creating microginins which may not be found in nature.

TECHNICAL FIELD

The present invention relates to the fields of chemistry, biology, biochemistry, molecular biology. The invention provides for novel nucleic acid molecules enabling the synthesis of microginin and microginin analogues. Microginin finds an application in therapeutics. The invention thus extends into the field of mammalian therapeutics and drug development.

INTRODUCTION Cyanobacteria and Microginin

Cyanbacteria are gram-negative bacteria. Due to their ability to perform photosynthesis they were long thought to belong to the plant kingdom and were formerly classified as blue-green algae. Cyanbacteria have adapted to almost all ecological niches. Most of strains known up to date are found in fresh water lakes and oceans. In the last few years cyanobacteria have been recognised as a source for biologically active natural compounds.

Cyanobacteria are a group of microscopic organisms somewhere “in between” algae and bacteria and they are found in freshwater and marine areas throughout the world. Scientifically, they are considered to be bacteria, but because they can perform photosynthesis, they also used to be classified as “blue-green algae”.

Cyanobacterial peptides (cyanopeptides) are among the most ubiquitously found potentially hazardous natural products in surface waters used by humans. Though these substances are natural in origin, eutrophication (i.e. excessive loading with fertilising nutrients) has caused massive cyanobacterial proliferation throughout Europe. Thus, cyanopeptides now occur with unnatural frequency and concentration.

A large group among the diverse cyanopeptides are the oligopeptides (peptides with a molecular weight of <2 KD). But while specific cyanopeptides—e.g. microcystins and nodularins—are well studied and recognised as being causative for many animal poisonings and human illness, a substantial and increasing body of evidence points toward a decisive role of other potentially toxic cyanopeptides in the causation of both acute and chronic human illnesses.

Freshwater and marine cyanobacteria are known to produce a variety of bioactive compounds, among them potent hepatotoxins and neurotoxins. Many of the toxic species of cyanobacteria tend to massive proliferation in eutrophicated water bodies and thus have been the cause for considerable hazards for animal and human health. One of the most widespread bloom-forming cyanobacteria is the genus Microcystis, a well-known producer of the hepatotoxic peptide microcystin. Microcystins are a group of closely related cyclic heptapeptides sharing the common structure. So far, more than 80 derivatives of microcystins have been identified, varying largely by the degree of methylation, peptide sequence, and toxicity.

The traditional botanical code describes the genus Microcystis as a coccal, unicellular cyanobacterium that grows as mucilaginous colonies of irregularly arranged cells (under natural conditions, while strain cultures usually grow as single cells). According to this tradition, morphological criteria such as size of the individual cells, colony morphology, and mucilage characteristics are used for species delimitation within Microcystis (i.e., morphospecies). Microcystin-producing strains as well as strains that do not synthesize microcystin have been reported for all species within the genus Microcystis. However, whereas most field samples and strains of Microcystis aeruginosa and Microcystis viridis studied to date were found to contain microcystins, strains of M. wesenbergii, M. novaceckii, and M. ichthyoblabe have only sporadically been reported to contain microcystins.

Beside microcystins, various other linear and cyclic oligopeptides such as anabaenopeptins, aeruginosins, microginins and cyanopeptolins are found within the genus Microcystis (Namikoshi, M., and K. L. Rinehart. 1996. Bioactive compounds produced by cyanobacteria. J. Ind. Microbiol. 17:373-384.).

Similar to microcystins, these peptides possess unusual amino acids like 3-amino-6-hydroxy-2-piperidone (Ahp) in cyanopeptolins, 2-carboxy-6-hydroxyoctahydroindol (Choi) in aeruginosin-type molecules or 3-amino-2 hydroxy-decanoic acid (Ahda) in microginins and numerous structural variants also exist within these groups. These peptides show diverse bioactivities, frequently protease inhibition (Namikoshi, M., and K. L. Rinehart. 1996. Bioactive compounds produced by cyanobacteria. J. Ind. Microbiol. 17:373-384).

The occurrence of both microcystins and other oligopeptides such as anabaenopeptins, microginins and cyanopeptolins in natural Microcystis populations was recently demonstrated. It is well known that the species and genotype composition in natural Microcystis populations is heterogeneous, and both microcystin- and non-microcystin-containing strains have been isolated from the same sample. Just as strains producing microginin and strains not producing microginin have been found. These results suggest a considerable diversity of genotypes with different oligopeptide patterns in natural Microcystis populations.

By typing single Microcystis colonies, it was possible in 1999 to show for the first time that the actual peptide diversity in a natural population of this genus is extremely high. Many of the substances detected belong to well-known groups of cyanobacterial peptides like microcystins, anabaenopeptins, microginins, cyanopeptolins, and aeruginosins, of which many have been discovered in Microcystis spp. In addition, numerous unknown components have been detected in such colonies. However, the origin of these unknown components has yet to be investigated, since besides the observed epiphytic cyanobacteria and algae, heterotrophic bacteria are also known to be present in Microcystis colonies. Chemical screening of cyanobacterial samples (both from field samples and from culture strains) has demonstrated a wide variety of substances: e.g. an almost monospecific bloom of Planktothrix agardhii contained as many as 255 different substances, most of which were oligopeptides.

Thus, it may be concluded, that the situation with respect to the assignment of the capability of microginin production to certain species and strains, i.e. also a true understanding of the genotypes and species involved as well as their evolution has to date, not been possible. In fact PEPCY a research project supported by the European Commission concluded that present information shows that one species or “morphotype” (i.e. individuals with the same morphological characteristics) may comprise a range of genotypes that encode for different “chemotypes” (i.e. morphologically indistinguishable individuals containing different cyanopeptides).

ACE Inhibitors and Microginin

ACE catalyses the conversion of angiotensin I into angiotensin II within the mammalian renin-angiotensin system, leading to arterial stenosis, which in turn causes an increase of blood pressure. ACE inhibitors counteract this process and therefore play a role in human medicine as blood pressure lowering agents. Microginin is an important drug candidate for ACE inhibition. So far only 30 structural variants of microginin are known, making clinical development difficult.

Microginins are characterized by a decanoic acid derivate, 3-amino-2-hydroxy-decanoic acid (Ahda) at the N-terminus and a predominance of two tyrosine units at the C-terminus. They vary in length from 4 to 6 amino acids with the variability occurring at the C-terminal end (Microginins, zinc metalloprotease inhibitors from the cyanobacterium Microcystis aeruginosa, 2000, Tetrahedron 56:8643-8656). In the past it has only been possible by means of synthesis of 3-amino-2-hydroxy-decanoic acid to chemically generate microginin variants (J Org. Chem. 1999 Apr. 16; 64(8):2852-2859. AcyInitrene Route to Vicinal Amino Alcohols. Application to the Synthesis of (−)-Bestatin and Analogues. Bergmeier S C, Stanchina D M.) Alternatively cyanobacterial strains were screened for microginin activity, which was tedious and time consuming. It has so far not been possible to screen for strains efficiently due to the lack of species understanding and a methodology of efficiently distinguishing microginin producers from non-producers (see above). Further it was not possible to easily and efficiently alter and thus develop microginins in order to provide for a variety of lead compounds from which better ACE-inhibitors may be developed.

BRIEF DESCRIPTION OF THE INVENTION

From Microcystis aeruginosa a cluster of genes, spanning about 30 kbps has been isolated encoding a hybrid synthetase composed of non-ribosomal peptide synthetases (NRPS), polyketide synthases (PKS) and tailoring enzyme which as the inventors show is responsible for the biosynthesis of microginin. The strain from which this nucleic acid was first isolated by G. C. Kürzinger from Lake Pehlitz 1977].

The inventors provide for a biological system enabling not only the production of micoginins, the heterologous expression of microginin, but also a system for modifying microginin and thus developing so far unknown variants of microginin. The invention further provides for nucleic acids and methods for identifying strains which have the ability to produce microginin.

In particular the invention relates to one or more nucleic acids encoding a microginin synthetase enzyme complex with the following activities: an adenylation domain (A*) wherein, the adenylation domain comprises a peptide sequence according to SEQ ID NO. 1, an acyl carrier protein (ACP), an elongation module (EM) of polyketide synthases (PKS) comprising the following activities: (i) ketoacylsynthase (KS), (ii) acyl transferase (AT) (iii) acyl carrier protein (ACP2), an aminotransferase (AMT), three to five elongation modules (EM) of non-ribosomal peptide synthetases (NRPS) comprising the following activities: (i) condensation domain (C), (ii) adenylation domain (A), (iii) thiolation domain (T) and a thioesterase (TE).

DETAILED DESCRIPTION OF THE INVENTION

As outlined above the invention in particular relates to one or more nucleic acids encoding a microginin synthetase enzyme complex with the following activities: an adenylation domain (A*) wherein, the adenylation domain comprises a peptide sequence according to SEQ ID NO. 1, an acyl carrier protein (ACP), an elongation module (EM) of polyketide synthases (PKS) comprising the following activities: (i) ketoacylsynthase (KS), (ii) acyl transferase (AT) (iii) acyl carrier protein (ACP 2), an aminotransferase (AMT), three to five elongation modules (EM) of non-ribosomal peptide synthetases (NRPS) comprising the following activities: (i) condensation domain (C), (ii) adenylation domain (A), (iii) thiolation domain (T) and a thioesterase (TE).

The inventors have found that microginin is the product of non-ribosomal synthesis. It is important to understand that microginin as previously identified in nature may also in part have been the product of ribosomal synthesis and further processed via various enzymatic reactions.

It is important to note that the nucleic acid claimed herein, i.e. a microginin synthetase enzyme complex may also be present in organisms other organisms than Microcystis sp., such as Nostoc, Anabaena, Plankthotrix or Oscillatoria. The term microginin shall thus not limit the invention to such nucleic acids producing synthetase enzyme complexes resulting in peptides officially termed “microginin”.

Herein, an adenylation domain (A*) is understood to activate octanoic acid as an acyl adenylate and an acyl carrier protein (ACP) is understood to bind the octanoic acid adenylate as a thioester.

An elongation module (EM) of polyketide synthases (PKS) is also known e.g. from the Jamaicamide synthetase gene cluster isolated from Lyngbya majuscula (Chem. Biol. Vol. 11, 2004 pp 817-833. Structure and Biosynthesis of the Jamaicamides, new mixed polyketide-peptide neurotoxin from the marine cyanobacterium Lyngbya majuscula) herein comprises at least the following activities: (i) ketoacylsynthase (KS), (ii) acyl transferase (AT) and (iii) acyl carrier protein (ACP2). The AT is responsible for the recognition of malonyl-CoA, the KS is resposible for the Claisen-type-condensation of the activated octanoic acid adenylate with malonyl-CoA and the ACP2 is responsible for binding of the resulting decanoic acid. An aminotransferase (AMT) performs the β-amination of the decanoic acid.

The nucleic acid according to the invention may have three to five elongation modules (EM) of non-ribosomal peptide synthetases (NRPS) comprising at least the following activities: (i) condensation domain (C), (ii) adenylation domain (A), (iii) thiolation domain (T). The A is responsible for the activation of carboxyl groups of amino acids, the T is responsible for the binding and the transport of the activated intermediate, the C is responsible for the condensation of the activated amino acids with the growing peptide chain.

Finally the nucleic acid according to the invention shall contain a thioesterase (TE) activity which performs the clevage of the final product from the synthetase complex.

One may envision that the nucleic acid according to the invention is present in a vector or a bacterial chromosome, in which case one may envision that the portions designated above while being in one cell need not all, be in, or on, one molecule. It is essential to the invention however, that a cell meant to produce microginin synthetase enzyme complex contains the activities designated above in order to produce an enzyme complex according to the invention which in turn may produce a microginin. Thus, the invention also encompasses derivatives of the nucleic acid molecule as outlined above having the function of a microginin synthetase enzyme complex.

The molecule is characterized by a special adenylation domain (A*) which is unusual in that it is not similar to known adenlyation domains found in other molecules encoding non-ribosomal enzyme complexes such as the microcystin synthetase gene cluster (Chem. Biol. Vol. 7 2000, pp 753-764: Structural organisation of microcystin synthesis in Microcystis aeruginosa PCC 7806: In integrated peptide-polyketide-synthetase system) Molecules encompassed herein are those which carry this adenylation domain (A*) as depicted in SEQ ID NO. 1 and at least an ACP whereby this ACP may stem from another known non-ribosomal enzyme complex, at least one EM of PKS whereby this EM may stem from another known non-ribosomal enzyme complex comprising at least the following activities: (i) KS, (ii) AT (iii) ACP, an AMT whereby this AMT may stem from another known non-ribosomal enzyme complex three to five EMs comprising at least the following activities: (i) C, (ii) A, (iii) T whereby these EMs may stem from another known non-ribosomal enzyme complex and a TE whereby this TE may stem from another known non-ribosomal enzyme complex. Chimeras whereby parts of the above are on one or more vectors and or integrated in chromosomes are equally encompassed by the invention as long as all the components are in one cell.

The invention also pertains to isolated nucleic acid molecules encoding a microginin synthetase enzyme complex comprising an adenylation domain which is 85% identical to SEQ ID NO. 1, more preferred 90% identical to SEQ ID NO. 1 most preferred 95% identical to SEQ ID NO. 1. Sequence identity herein is in percent of total sequence of the adenylation domains when aligned with conventional nucleotide alignment software, such as the best fit and or pileup programs of the GCG package

The invention also pertains to a microginin synthetase enzyme protein complex with the following activities: an adenylation domain (A*) wherein, the adenylation domain comprises a peptide sequence according to SEQ ID NO. 1, an acyl carrier protein (ACP), an elongation module (EM) of polyketide synthases (PKS) comprising the following activities: (i) ketoacylsynthase (KS), (ii) acyl transferase (AT) (iii) acyl carrier protein (ACP 2), an aminotransferase (AMT), three to five elongation modules (EM) of non-ribosomal peptide synthetases (NRPS) comprising the following activities: (i) condensation domain (C), (ii) adenylation domain (A), (iii) thiolation domain (T) and a thioesterase (TE).

The invention in particular also relates to a nucleic acid molecule encoding an adenylation domain (A*) wherein, the adenylation domain comprises a peptide sequence according to SEQ ID NO. 1.

The invention in particular also relates to a peptide molecule, an adenylation domain (A*) wherein, the molecule comprises a peptide sequence according to SEQ ID NO. 1.

The invention in particular also relates to a nucleic acid molecule encoding an adenylation domain (A*) wherein, the molecule comprises a nucleic acid sequence according to SEQ ID NO. 25.

In a preferred embodiment of the invention the nucleic acid additionally and optionally comprises sequences encoding the following activities or domains: a monooxygenase (MO), an integrated N-methyltransferase domain (MT) within one or more elongation modules (EM) of NRPS, a non-integrated N-methyltrasferase (MT), a modifying activity (MA) wherein, said MA is selected from the group comprising the following activities: halogenase, sulfatase, glycosylase, racemase, O-methyltransferase and C-methyltransferase, two or more peptide repeat spacer sequences (SP) consisting of one or more repeats of being either glycine rich or proline and leucine rich, located adjacently upstream and downstream of the MO and/or another MA.

Herein MO is an enzyme catalyzing the hydroxylation of the decanoic acid, an integrated N-methyltransferase domain (MT) within one or more elongation modules (EM) of NRPS catalyses the methylation of the amide bond by the respective module and a non-integrated N-methyltrasferase (MT) catalyzes the methylation of an amino group of the microginin. The term modifying enzyme stands for numerous enzymes such enzymes may add groups or create bonds, in a preferred embodiment MA is selected from the group comprising the following activities: halogenase, sulfatase, glycosylase, racemase, O-methyltransferase and C-methyltransferase.

Nucleic acids encoding two or more peptide repeat spacer sequences (SP) consisting of one or more repeats being either glycine rich or proline and leucine rich have astonishingly been found by the inventors to aid in integration of novel MAs into existing microginin synthetase enzyme complexes. By means of placing such SPs adjacently to MAs the inventors are able to create microginin synthetase enzyme complexes (MSEC) comprising activities previously not found in MSECs. This in turn allows for the creation of novel microginins with potentially novel therapeutic properties. Thus the invention relates to nucleic acids encoding two or more peptide repeat spacer sequences (SP) consisting of one or more repeats being either glycine rich or proline and leucine rich may be positioned adjacently to a MA such as but not limited to a halogenase, a sulfatase, a glycosylase, a racemase, an O-methyltransferase or a C-methyltransferase. These SPs aid in ensuring that the “foreign” activity “works” in the enzyme complex. The inventors have found, that this is due to the lack of secondary structures in the SP peptide chains.

The nucleic acid according to the invention in a preferred embodiment optionally comprises the following sequences, nucleic acid sequences encoding protein sequences as follows:

An adenylation domain (A*) according to SEQ ID NO. 1, an acyl carrier protein (ACP) according to SEQ ID NO. 2, an elongation module of polyketide synthases responsible for the activation and the condensation of malonyl-Co A: (i) ketoacylsynthase domain (KS) according to SEQ ID NO. 3, (ii) acyl transferase domain (AT) according to SEQ ID NO. 4, an acyl carrier protein domain (ACP 2) according to SEQ ID NO. 5, an aminotransferase (AMT) according to SEQ ID NO. 6, an elongation modules of non-ribosomal peptide synthetases responsible for the activation and condensation of alanin: (i) condensation domain (C) according to SEQ ID NO. 7, (ii) adenylation domain (A) according to SEQ ID NO. 8, (iii) thiolation domains (T) according to SEQ ID NO. 9, an elongation modules of non-ribosomal peptide synthetases responsible for the activation and condensation of leucin: (i) condensation domain (C2) according to SEQ ID NO. 10, (ii) adenylation domain (A 2) according to SEQ ID NO. 11, (iii) thiolation domain (T 2) according to SEQ ID NO. 12, an elongation modules of non-ribosomal peptide synthetases responsible for the activation and condensation of tyrosine 1: (i) condensation domain (C 3) according to SEQ ID NO. 13, (ii) adenylation domain (A 3) according to SEQ ID NO. 14 (iii) thiolation domain (T 3) according to SEQ ID NO. 15, an elongation modules of non-ribosomal peptide synthetases responsible for the activation and condensation of tyrosine 2: (i) condensation domain (C4) according to SEQ ID NO. 16, (ii) adenylation domain (A 4) according to SEQ ID NO. 17, (iii) thiolation domain (T 4) according to SEQ ID NO. 18, a thioesterase (TE) according to SEQ ID NO. 19, a monooxygenase (MO) according to SEQ ID NO. 20, two or more peptide repeat spacer sequences (SP1/SP2) according to SEQ ID NO. 21 and 22, an integrated N-methyltransferase domain (MT) within the elongation module (EM) of the NRPS responsible for the activation and condensation of leucin according to SEQ ID 23 and a non-integrated N-methyltrasferase (MT 2) according to SEQ ID NO. 24.

As outlined above, the minimal requirement according to the invention is a nucleic acid encoding a microginin synthetase enzyme complex with the following activities: an adenylation domain (A*) wherein, the adenylation domain comprises a peptide sequence according to SEQ ID NO. 1, an ACP according to SEQ ID NO. 2, an elongation module (EM) of polyketide synthases (PKS) comprising the following activities: (i) ketoacylsynthase (KS) according to SEQ ID NO. 3, (ii) acyl transferase (AT) according to SEQ ID NO 4, (iii) acyl carrier protein (ACP 2) according to SEQ ID NO. 5, an aminotransferase (AMT) according to SEQ ID NO. 6, three to five elongation modules (EM) of non-ribosomal peptide synthetases (NRPS) comprising the following activities: (i) condensation domain (C) according to SEQ ID NO. 7, (ii) adenylation domain (A) according to SEQ ID NO. 8, (iii) thiolation domain (T) according to SEQ ID NO. 9 and a thioesterase (TE) according to SEQ ID NO. 10. A molecule comprising the above sequences is preferred herein.

The invention explicitly also relates to analogs hereto, additionally comprising, e.g. other activities and/or spacer regions both transcribed and non-transcribed.

It is apparent to those skilled in the art, that amino acids may be exchanged maintaining the enzymatic activity required. Thus, the invention also relates to molecules with sequences which are not identical to those outlined above however, altered only in so far as the enzymatic activity desired is retained.

The nucleic acid according to the invention may contain nucleic acids selected from the group comprising: an adenylation domain (A*) according to SEQ ID NO. 25, an acyl carrier protein (ACP) according to SEQ ID NO. 26, an elongation module of polyketide synthases encoding for the activation and the condensation of malonyl-Co A: (i) ketoacylsynthase domain (KS) according to SEQ ID NO. 27, (ii) acyl transferase domain (AT) according to SEQ ID NO. 28, (iii) acyl carrier protein domain (ACP 2) according to SEQ ID NO. 29, an aminotransferase (AMT) according to SEQ ID NO. 30, an elongation modules of non-ribosomal peptide synthetases encoding for the activation and condensation of alanin: (i) condensation domain (c) according to SEQ ID NO. 31, (ii) adenylation domain (A) according to SEQ ID NO. 32, (iii) thiolation domain (T) according to SEQ ID NO. 33, an elongation modules of non-ribosomal peptide synthetases encoding for the activation and condensation of leucin: (i) condensation domain (C 2) according to SEQ ID NO. 34, (ii) adenylation domain (A 2) according to SEQ ID NO. 35, (iii) thiolation domain (T 2) according to SEQ ID NO. 36, elongation modules of non-ribosomal peptide synthetases encoding for the activation and condensation of tyrosine 1: (i) condensation domains (C3) according to SEQ ID NO. 37, (ii) adenylation domains (A 3) according to SEQ ID NO. 38, (iii) thiolation domains (T 3) according to SEQ ID NO. 39, elongation modules of non-ribosomal peptide synthetases encoding for the activation and condensation of tyrosine 2: (i) condensation domains (C4) according to SEQ ID NO. 40, (ii) adenylation domains (A 4) according to SEQ ID NO. 41, (iii) thiolation domains (T 4) according to SEQ ID NO. 42, a thioesterase (TE) according to SEQ ID NO. 43, a monooxygenase (MO) according to SEQ ID NO. 44, two or more peptide repeat spacer sequences (SP1/2) according to SEQ ID NO. 45 and 46, an integrated N-methyltransferase domain (MT) within the elongation module (EM) of the NRPS encoding for the activation and condensation of leucin according to SEQ ID 47 and a non-integrated N-methyltrasferase (MT 2) according to SEQ ID NO. 48.

As outlined above, the minimal requirement according to the invention is a nucleic acid encoding a microginin synthetase enzyme complex with the following activities: an adenylation domain (A*) wherein, the adenylation domain is a nucleic acid sequence according to SEQ ID NO. 25, an ACP with a nucleic acid sequence according to SEQ ID NO. 26, an elongation module (EM) of polyketide synthases (PKS) comprising the following activities: (i) ketoacylsynthase (KS) with a nucleic acid sequence according to SEQ ID NO. 27, (ii) acyl transferase (AT) with a nucleic acid sequence according to SEQ ID NO 28, (iii) acyl carrier protein (ACP 2) with a nucleic acid sequence according to SEQ ID NO. 29, an aminotransferase (AMT) with a nucleic acid sequence according to SEQ ID NO. 30, three to five elongation modules (EM) of non-ribosomal peptide synthetases (NRPS) comprising the following activities: (i) condensation domain (C) with a nucleic acid sequence according to SEQ ID NO. 31, (ii) adenylation domain (A) with a nucleic acid sequence according to SEQ ID NO. 32, (iii) thiolation domain (T) with a nucleic acid sequence according to SEQ ID NO. 33 and a thioesterase (TE) with a nucleic acid sequence according to SEQ ID NO. 43. A molecule comprising the above sequences is preferred herein.

The invention also relates to nucleic acid molecules with sequences which are not identical to those outlined above however, altered only in so far as the enzymatic activity desired is retained. I particular one skilled in the art will know that positions in nucleic acid triplets may “wobble” and these positions may thus be altered with no influence on the peptide sequence. Further multiple amino acids are encoded by more than one DNA triplet. One skilled in the art will know that one may alter such triplets maintaining the amino acid sequence. Thus said sequences are equally encompassed by the invention.

The invention also pertains to isolated nucleic acid molecules encoding a microginin synthetase enzyme complex comprising an adenylation domain which is 85% identical to SEQ ID NO. 25, more preferred 90% identical to SEQ ID NO. 1 most preferred 95% identical to SEQ ID NO. 1. Sequence identity herein is in percent of total sequence of the adenylation domains when aligned with a conventional amino acid alignment software such as the best fit and or pileup programs of the GCG package.

In a preferred embodiment the one or more nucleic acids according to the invention are organized in sequence parts encoding the microginin synthetase enzyme complex in an upstream to downstream manner as depicted in FIG. 1. In a particularly preferred embodiment the activities and domains are arranged as shown and on one molecule.

The nucleic acid molecule may be part of a vector. Such vectors are in particular, bacterial artificial chromosomes (BAC), Cosmids or Fosmids, and Lambda vectors. Preferred plasmid vectors which are able to replicate autonomously in cyanobacteria are derived from the pVZ vectors. Preferred fosmid vectors which are able to replicate autonomously in cyanobacteria are derived from the pCC1FOS™ and pCC2FOS™ vectors (Epicentre Biotechnologies). The integration of the nucleic acid according to the invention into the vector is a procedure known to those skilled in the art (Molecular Cloning: A Laboratory manual, 1989, Cold Spring Harbour Labaratory Press) or in the manuals of manufactures of kits for creation of genomic libraries (e.g. Epicenter Biotechnologies).

In a preferred embodiment the invention concerns a microorganism transformed with a nucleic acid according to the invention. The nucleic acid according to the invention may integrated into the chromosome of the host organism or may present on a separate vector (see also examples). It is preferred that the phototrophic cyanobacterial host organism is selected for the group comprising: Synechocystis sp., Synechococcus sp., Anabaena sp., Nostoc sp., Spirulina sp., Microcystis sp . . . . Cells are cultured as follows:

Media: Bg 11 (for cultivation of cyanobacteria) Aeration: air containing 0.3-3.0% carbon dioxide Light intensity: 40-100 μE/m²*s (diameter of illuminated culture vessels of photobioreactor d=4-12 cm) Cell density at harvest: OD₇₅₀1-2 And if the host is Microcystis aeruginosa: Light quality: Additional red light illumination with 25 μE/m²*s for 24-48 hours before harvesting.

It is preferred that the heterotrophic host organism is selected for the group comprising: E. coli and Bacillus sp. due to a more suitable GC content and codon usage than other heterotrophic bacteria.

In case of using E. coli for the heterologues expression of the microginin synthetase a phosphopanthetein transferase (Ppt) has to be co-expressed in order to enable the synthesis of microginin. The co-expression of the Ppt from a microginin producing strain would be preferred. Other Ppt's with a broad specificity even from heterotophic organisms like Bacillus sp. are also suitable.

In one embodiment of the invention the invention relates to a method of producing a microginin, comprising culturing a cell under conditions under which the cell will produce microginin, wherein said cell comprises a nucleic acid encoding a recombinant microginin, according to the invention, and wherein said cell does not produce the microginin in the absence of said nucleic acid.

The inventors have identified nucleic acid sequences which for the first time make it possible to detect nucleic acids encoding a microginin synthetase enzyme complex. This has been extremely difficult, due to the fact that other gene clusters which encode non-ribosomal protein producing complexes share sequence similarity with the present cluster claimed herein. Such primers or probes according to the invention are selected from the group of, a) nucleic acid according to SEQ ID NO. 49 (Primer A), b) nucleic acid according to SEQ ID NO. 50 (Primer B), c) nucleic acid according to SEQ ID NO. 51 (Primer C), d) nucleic acid according to SEQ ID NO. 52 (Primer D), e) nucleic acid according to SEQ ID NO. 53 (Primer E), f) nucleic acid according to SEQ ID NO. 54 (Primer F), g) nucleic acid according to SEQ ID NO. 55 (Primer G), h) nucleic acid according to SEQ ID NO. 56 (Primer H), i) nucleic acid according to SEQ ID NO. 57 (Primer I) and j) nucleic acid according to SEQ ID NO. 58 (Primer J). It is known to one skilled in the art that such primers or probes may be altered slightly and still accomplishes the task of specifically detecting the desired target sequence. Such alterations in sequence are equally encompassed by the invention. The primers or probes according to the invention may be applied in hybridization reactions and/or amplification reactions. Such reactions are known to one skilled in the art.

The invention also concerns a method for detecting a microginin synthetase gene cluster in a sample wherein, one or more of the nucleic acids according to the invention are, applied in an amplification and/or a hybridization reaction.

In a preferred embodiment of the method according to the invention primers D and F or H and J or E and I or E and A are added to a PCR reaction mixture comprising a sample and wherein, presence of an amplification product represents presence of microginin synthetase gene cluster and absence of an amplification product represents absence of a microginin synthetase gene cluster. As can be seen from the examples (example 3 below), certain combinations are preferred. Samples may be isolated DNA, prokaryotic cells stemming from plates or liquid cultures.

When performing an amplification reaction with primers D and F the most preferred amplification conditions are as follows: a) denaturing, b) 48° C. annealing and c) elongation (product size: 675 bp). These temperatures may vary a bit in the range of 2-8 degrees C.

When performing an amplification reaction with primers H and J the most preferred amplification conditions are as follows: a) denaturing, b) 54° C. annealing and c) elongation (product size: 1174 bp). These temperatures may vary a bit in the range of 2-8 degrees C.

When performing an amplification reaction with primers E and I the most preferred amplification conditions are as follows: a) denaturing, b) 56° C. annealing and c) elongation (product size: 1279 bp). These temperatures may vary a bit in the range of 2-8 degrees C.

When performing an amplification reaction with primers E and A the most preferred amplification conditions are as follows: a) denaturing, b) 57° C. annealing and c) elongation (product size: 621 bp). These temperatures may vary a bit in the range of 2-8 degrees C. Molarity is most commonly 0.2-1.0 μM for the primers. Buffers and other reagents depending on polymerase used.

When performing hybridisation reactions the above nucleic acids are usually labeled. Such labels may be radioactive or non-radioactive, such as fluorescent. The nucleic acid primers or probes may be applied, e.g. for the screening of libraries.

The invention also relates to antibodies against a peptide according to SEQ ID NO. 1 (A*).

The creation of such antibodies is known to one skilled in the art. The antibodies may be polyclonal or monoclonal. Such antibodies may be labeled or non-labeled, they may also be altered in other form, such as humanized.

The inventors have astonishingly found that newly identified peptide repeat spacer sequences (SP) may be placed adjacently to MAs I in order to create novel hybrid gene clusters. These SPs act by spacing the novel activity or domain so that it is functionally active in the microginin synthetase enzyme complex.

The invention thus, further relates to nucleic acids encoding a peptide repeat spacer sequence (SP) wherein, the peptide sequence comprises at least 4 glycin amino acids per single repeat unit (SRU) or, at least 5 proline and/or leucin amino acids per SRU. A SRU within the SP is between 7 and 15 amino acids in length and, the SP comprises between 2 and 10 SRUs.

The invention further relates to peptides of a peptide repeat spacer sequence (SP) wherein, the peptide sequence comprises at least 4 glycin amino acids or, at least 5 proline and/or leucin amino acids, the single repeat unit (SRU) within the SP is between 7 and 15 amino acids in length and, the SP comprises between 2 and 10 SRU. In a preferred embodiment of the invention the SRU is between 9 and 13 amino acids in length in a particularly preferred embodiment the SRU is eleven amino acids in length. In a preferred embodiment the SP comprises between 3 and 9 SRU.

In a preferred embodiment the nucleic acid encoding the peptide repeat spacer sequence (SP) according to the invention, encodes a peptide SRU as shown in SEQ ID NO. 20 or SEQ ID NO. 21. In a further embodiment the peptide repeat spacer sequence (SP) according to the invention, comprises or contains a sequence as shown in SEQ ID NO. 20 or SEQ ID NO. 21. In a further embodiment the nucleic acid according to the invention has a sequence as laid down in SEQ ID NO. 43 or SEQ ID NO. 44.

Not only by means of the above mentioned SPs but in particular because of these the inventors are able to create enzyme complexes resulting in microginin variants which may not be found in nature. This is an essential aspect of the present invention. The invention provides for, for the first time a simple method of producing recombinant microginin variants comprising, modifying the nucleic acid according to the invention in vitro or in vivo, growing a recombinant cell comprising said recombinantly modified nucleic acid encoding a microginin synthetase under conditions which lead to synthesis of a microginin and, recovering the synthesized microginin.

In a preferred embodiment of said method according to the invention, said modifying of said nucleic acid may be an action selected from the group of one or more of the following actions: a) inactivation of one or more of the MTs present, b) substitution of one or more of the MTs present with a halogenase, a sulfatase, a glycosylase, a racemase, an O-methyltransferase or a C-methyltransferase, c) inactivation of the MO, d) substitution of the MO with a halogenase, a sulfatase, a glycosylase, a racemase, an O-methyltransferase or a C-methyltransferase, e) inactivation of the AMT, f) substitution of the AMT with a halogenase, a sulfatase, a glycosylase, a racemase, an O-methyltransferase or a C-methyltransferase, g) inactivation of the PKS module, h) substitution of the entire PKS module with an alternative PKS module and/or substitution of one or more of the domains (KS, AT, ACP) therein, i) inactivation of the A* domain, j) substitution of the A* domain with alternative A domains, k) inactivation of one or more of the NRPS modules and 1) substitution of one or more of the NRPS modules with alternative NRPS modules and/or substitution of one or more of the domains (C, A, T) therein.

Halogenases, sulfatases, glycosylases, racemases, O-methyltransferases or C-methyltransferases are known from prokaryotes. These enzymes are encoded by genes of the secondary metabolism in particular NRPS/PKS systems.

Alternative PKS-systems, entire modules as well as single domains (KS, AT, ACP) are found in cyanobacteria as well as Actinomycetes, Myxobacteria, Bacillus among the bacteria.

Alternative NRPS-systems, entire modules as well as single domains (C, A, T) are found in cyanobacteria as well as Actinomycetes, Myxobacteria, Bacillus among the bacteria.

In a preferred embodiment the above are from cyanobacteria.

It is important to note, that said inactivation and/or substitution may done in many ways, e.g. inactivation may imply deleting the complete activity or domain, or may imply inactivation by means of a single nucleotide exchange.

The methods are known to those skilled in the art and comprise basic molecular biological methods such as DNA isolation, restriction digestion, ligation, transformation, amplification etc.

In a preferred embodiment said alternative modules or domains which are used for substitution of the original module or domain, additionally may comprise one or more SP nucleic acids according to the invention located adjacently upstream of the module or domain used for substitution and one or more SP nucleic acids according the invention located adjacently downstream of the module or domain used for substitution. Thus, in this embodiment of the invention a construct is made comprising the domain which is to be entered into the original nucleic acid according to the invention, further comprising one or more SPs located adjacently in an upstream and downstream manner. This construct is then ligated into the original microginin synthetase encoding nucleic acid. The resultant construct is then brought into a host by means of transformation for either a) integration into the host chromosome or b) with a self-replicating vector.

The polypeptides, i.e. proteins can be any of those described above but with not more than 10 (e.g., not more than: 10, nine, eight, seven, six, five, four, three, two, or one) conservative substitutions. Conservative substitutions are known in the art and typically include substitution of, e.g. one polar amino acid with another polar amino acid and one acidic amino acid with another acidic amino acid. Accordingly, conservative substitutions preferably include substitutions within the following groups of amino acids: glycine, alanine, valine, proline, isoleucine, and leucine (non polar, aliphatic side chain); aspartic acid and glutamic acid (negatively charged side chain); asparagine, glutamine, methionine, cysteine, serine and threonine (polar uncharged side chain); lysine, histidine and arginine; and phenylalanine, tryptophane and tyrosine (aromatic side chain); and lysine, arginine an histidine (positively charged side chain). It is well known in the art how to determine the effect of a given substitution, e.g. on pK₁ etc. All that is required of a polypeptide having one or more conservative substitutions is that it has at least 50% (e.g., at least: 55%; 60%; 65%, 70%; 75%; 80%; 85%; 90%; 95%; 98%; 99%; 99.5%; or 100% or more) of the ability of the unaltered protein according to the invention.

In preferred embodiments the polynucleotides, i.e. nucleic acids of the present invention also comprise nucleic acid molecules which are at least 85%, preferably 86%, 87%, 88%, 89%, 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98%, or 99% identical to those claimed herein.

The determination of percent identity between two sequences is accomplished using the mathematical algorithm of Karlin and Altschul (1993) Proc. Natl. Acad. Sci. USA 90: 5873-5877. Such an algorithm is incorporated into the BLASTN and BLASTP programs of Altschul et al. (1990) J. Mol. Biol. 215: 403-410. BLAST nucleotide searches are performed with the BLASTN program, score=100, word length=12, to obtain nucleotide sequences homologous to the nucleic acids according to the invention. BLAST protein searches are performed with the BLASTP program, score=50, wordlength=3, to obtain amino acid sequences homologous to the EPO variant polypeptide, respectively. To obtain gapped alignments for comparative purposes, Gapped BLAST is utilized as described in Altschul et al. (1997) Nucleic Acids Res. 25: 3389-3402. When utilizing BLAST and Gapped BLAST programs, the default parameters of the respective programs are used.

FIGURES

FIG. 1 depicts the structure of microginin.

FIG. 2 depicts the microginin synthetase gene cluster and the biosynthetic pathway of microginin.

EXAMPLES Example 1 Method for Detecting Gene Clusters According to the Invention

Strains carrying a gene cluster encoding a microginin synthetase complex can be distinguished from strains not carrying such a gene cluster performing a PCR reaction using RedTaq ReadyMix PCR Reaction Mix with MgCl₂ (Sigma) and primer pairs and the corresponding annealing temperatures as described in claims 11-12. In particular the PCR conditions are as follows: an initial denaturation for 1 minutes at 95° C., followed by 30 cycles of denaturation at 95° C. for 30 seconds, elongation at said annealing temperatures for 30 seconds and extension at 72° C. for 1 kb of product size.

Example 2 Method for Optimised Cultivation of Microginin Producing Microcystis spp

Strains. Media: Bg 11 (for cultivation of cyanobacteria) Aeration: air containing 0.3-3.0% carbon dioxide Light intensity: 40-100 pE/m²*s (diameter of illuminated culture vessels of photobioreactor d=4-12 cm) Light quality: Additional red light illumination with 25 μE/m²*S for 24-48 hours before harvesting. Cell density at harvest: OD_(750nm) 1-2

Tables

TABLE 1 SEQ ID MTINYGDLQEPFNKFSTLVELLRYRASSQPERLAYIFLRDGEIE NO. 1 EARLTYGELDQKARAIAAYLQSLEAEGERGLLLYPPGLDFISAF A* FGCLYAGVVAIPAYPPRRNQNLLRLQAIIADSQARFTFTNAALF PSLKNQWAKDPELGAMEWIVTDEIDHHLREDWLEPTLEKNSLAF LQYTSGSTGTPKGVMVSHHNLLINSADLDRGWGHDQDSVMVTWL PTFHDMGLIYGVIQPLYKGFLCYMMSPASFMERPLRWLQALSDK KATHSAAPNFAYDLCVRKIPPEKRATLDLSHWCMALNGAEPVRA EVLKKFAEAFQVSGFKATALCPGYGLAEATLKVTAVSYDSPPYF YPVQANALEKNKIVGATETDTNVQTLVGCGWTTIDTQIVIVNPE TLKPCSPEIVGEIWVSGSTIAQGYWGKPQETQETFQAYLADTGA GPFLRTGDLGFIKDGELFITGRLKEIILIRGRNNYPQDIELTVQ NSHPALRPSCGAAFTVENKGEEKLVVVQEVERTWLRKVDIDEVK RAIRKAVVQEYDLQVYAIALIRTGSLPKTSSGKIQRRSCRAKFL EGSLEILG SEQ ID MSTEIPNDKKQPTLTKIQNWLVAYMTEMMEVDEDEIDLSVPFDE NO. 2 YGLDSSMAVALIADLEDWLRRDLHRTLIYDYPTLEKLAKQVSEP ACP SEQ ID MEPIAIIGLACRFPGADNPEAFWQLMRNGVDAIADIPPERWDIE NO. 3 RFYDPTPATAKKMYSRQGGFLKNVDQFDPQFFRISPLEATYLDP KS QQRLLLEVTWEALENAAIVPETLAGSQSGVFIGISDVDYHRLAY QSPTNLTAYVGTGNSTSIAANRLSYLFDLRGPSLAVDTACSSSL VAVHLACQSLQSQESNLCLVGGVNLILSPETTVVFSQARMIAPD SRCKTFDARADGYVRSEGCGVVVLKRLRDAIQDGDRILAVIEGS AVNQDGLSNGLTAPNGPAQQAVIRQALANAQVKPAQISYVEAHG TGTELGDPIEVKSLKAVLGEKRSLDQTCWLGSVKTNIGHLEAAA GMAGLIKVVLCLQHQEIPPNLHFQTLNPYISLADTAFAIPTQAQ PWRTKPPKSGENGVERRLAGLSSFGFGGTNSHVIL SEQ ID VFLFAGQGSQYVGMGRQLYETQPIFRQTLDRCAEILRPHLDQPL NO. 4 LEILYPADPEAETASFYLEQTAYTQPTLFAFEYALAQLWRSWGI AT EPAAVIGHSVGEYVAATVAGALSLEEGLTLIAKRAKLMQSLPKN GTMIAVFAAEERVKAVIEPYRTDVAIAAVNGPENFVISGKAPII AEIIIHLTAAGIEVRLPLKVSHAFHSHLLEPILDSLEQEAAAIS YQPLQIPLVANLTGEVLPEGATIEARYWRNHARNPVQFYGSIQT LIEQKFSLFLEVSPKPTLSRLGQQCCPERSTTWLFSLALPPQEE EQSLLNSLAILYDSQGAE SEQ ID ITLQTLVGNLLQLSPADVNVHTPFLEMGADSIVMVEAVRRIENT NO. 5 YNVKIAMRQLFEELSTLDALATYL ACP 2 SEQ ID KEMLYPIVAQRSQGSRIWDVDGNEYIDMTMGQGVTLFGHQPDFI NO. 6 MSALQSQLTEGIHLNPRSPIVGEVAALICELTGAERACFCNSGT AMT EAVMAAIRIARATTGRSKIALFEGSYHGHADGTLFRNQIIDNQL HSFPLALGVPPSLSSDVVVLDYGSAEALNYLQTQGQDLAAVLVE PIQSGNPLLQPQQFLQSLRQITSQMGIALIFDEMITGFRSHPGG AQALFGVQADIATYGKVVAGGMPIGVIAGKAHYLDSIDGGMWRY GDKSYPGVDRTFFGGTFNQHPLAMVAARAVLTHLKEQGPGLQQQ LTERTAALADTLNHYFQAEEVPIKIEQFSSFFRFALSGNLDLLF YHMVEKGIYVWEWRKHFLSTAHTEADLAQFVQAVKDSITELR SEQ ID GGDQVPLTEAQRQLWILAQLGDNGSVAYNQSVTLQLSGPLNPVA NO. 7 MNQAIQQISDRHEALRTKINAQGDSQEILPQVEINCPILDFSLD C QASAQQQAEQWLKEESEKPFDLSQGSLVRWHLLKLEPELHLLVL TAHHIISDGWSMGVILRELGELYSAKCQGVTANLKTPKQFRELI EWQSQPSQGEELKKQQAYWLATLADPPVLNLPTDKPRPALPSYQ ANRRSLTLDSQFTEKLKQFSRKQGCTLLMTLLSVYNILVHRLTG QDDILVGLPASGRGLLDSEGMVGYCTHFLPIRSQLA SEQ ID TYSELNCRANQLALHYLQKLGVGPEVLVGILVERSLEMIVGLLG NO. 8 ILKAGGAYVPLDPDYPPERLQFMLEDSQFFLLLTQQHLLESFAQ A SSETATPKIICLDSDYQIISQAKNINPENSVTTSNLAYVIYTSG STGKPKGVMNNHVAISNKLLWVQDTYPLTTEDCILQKTPFSFDV SVWELFWPLLNGARLVFAKPNGHKDASYLVNLIQEQQVTTLHFV SSMLQLFLTEKDVEKCNSLKRVICSGEALSLELQERFFARLVCE LHNLYGPTEAAIHVTFWQCQSDSNLKTVPIGRPIANIQIYILDS HLQPVPIGVIGELHIGGVGLARGYLNRPELTAEKFIANPFASLD PPLTPLDKGGDESYKTFKKGGEQPSRLYKTGDLARYLPDGKIEY LGRIDNQVKIRGFRIELGEIEAVLLSHPQVREAVV SEQ ID EAIAAIFGQVLKLEKVGIYDNFFEIGGNSLQATQVISRLRESFA NO. 9 LELPLRRLFEQPTVADLALAV T SEQ ID PRDGQLPLSFAQSRLWFLYQLEGATGTYNMTGALSLSGPLQVEA NO. 10 LKQALRTIIQRHEPLRTSFQSVDGVPVQVINPYPVWELAMVDLT C2 GKETEAEKLAYQESQTPFDLTNSPLLRVTLLKLQPEKHILLINM HHIISDGWSIGVFVRELSHLYRAFVAGKEPTLPILPIQYADFAV WQREWLQGKVLAAQLEYWKRQLADAPPLLELPTDRPRPAIQTFQ GKTERFELDRKLTQELKALSQQSGCTLFMTLLAAFGVVLSRYSG QTDIVIGSAIANRNRQDIEGLIGFFVNTLALRLDLS SEQ ID TYGELNHRANQLAHYLQSLGVTKEQIVGVYLERSLEMAIGFLGI NO. 11 LKAGAAYLPIDPEYPSVRTQFILEDTQLSLLLTQAELAEKLPQT A2 QNKIICLDRDWPEITSQPQTNLDLKIEPNNLAYCIYTSGSTGQP KGVLISHQALLNLIFWHQQAFEIGPLHKATQVAGIAFDATVWEL WPYLTTGACINLVPQNILLSPTDLRDWLLNREITMSFVPTPLAE KLLSLDWPNHSCLKTLLLGGDKLHFYPAASLPFQVINNYGPTEN TVVATSGLVKSSSSHHFGTPTIGRPIANVQIYLLDQNLQPVPIG VPGELHLGGAGLAQGYLNRPELTAEKFIANPFDPPLTPLDKGGE EPSKLYKTGDLARYLPDGNVEFLGRIDNQVKIRGFRIETGEIEA VLSQYFLLAESVV SEQ ID AQLTQIWSEVLGLERIGVKDNFFELGGHSLLATQVLSRINSAFG NO. 12 LDLSVQIMFESPTIAGIAGYI T2 SEQ ID ARDGHLPLSFAQQRLWFLHYLSPDSRSYNTLEILQIDGNLNLTV NO. 13 LEQSLGELINRHEIFRTTFPTVSGEPIQKIALPSRFQLKVDNYQ C3 DLDENEQSAKIQQVAELEAGQAFDLTVGPLIQFKLLQLSPQKSV LLLKMHHIIYDGWSFGILIRELSALYEAFLKNLANPLPALSIQY ADFAVWQRQYLSGEVLDKQLNYWQEQLATVSPVLTLPTDRPRPA IQTFQGGVERFQLDQNVTQGLKKLGQDQVATLFMTLLAGFGVLL SRYSGQSDLMVGSPIANRNQAAIEPLIGFFANTLALRINLS SEQ ID TYTELNHRANQLAHYLQTLGVGAEVLVGISLERSLEMIIGLLGI NO. 14 LKVGGAYLPLDPDYPTERLQLMLEDSQVPFLITHSSLLAKLPPS A3 QATLICLDHIQEQISQYSPDNLQCQLTPANLANVIYTSGSTGKP KGVMVEHKGLVNLALAQIQSFAVNHNSRVLQFASFSFDACISEI LMTFGSGATLYLAQKDALLPGQPLIERLVKNGITHVTLPPSALV VLPQEPLRNLETLIVAGEACSLDLVKQWSIDRNFFNAYGPTEAS VCATIGQCYQDDLKVTIGKAIANVQIYILDAFLQPVPVGVSGEL YIGGVGVARGYLNRPELTQEKFIANPFSNDPDSRLYKTGDLARY LPDGNIEYLGRIDNQVKIRGFRIELGEIEAVLSQCPDVQNTAV SEQ ID EILAQIWGQVLKIERVSREDNFFELGGHSLLATQVMSRLRETFQ NO. 15 VELPLRSLFTAPTIAELALTI T3 SEQ ID NDSANLPLSFAQQRLWFLDQLEPNSAFYHVGGAVRLEGTLNITA NO. 16 LEQSLKEIINRHEALRTNFITIDGQATQIIHPTINWRLSVVDCQ C4 NLTDTQSLEIAEAEKPFNLAQDCLFRATLFVRSPLEYHLLVTMH HIVSDGWSIGVFFQELTHLYAVYNQGLPSSLTPIKIQYADFAVW QRNWLQGEILSNQLNYWREQLANAPAFLPLPTDRPRPAIQTFIG SHQEFKLSQPLSQKLNQLSQKHGVTLFMTLLAAFATLLYRYTGQ ADILVGSPIANRNRKEIEGLIGFFVNTLVLRLSLD SEQ ID TYAELNHQANQLVHYLQTLGIGPEVLVAISVERSLEMIIGLLAI NO. 17 LKACGAYLPLAPDYPTERLQFMLEDSQASFLITHSSLLEKLPSS A4 QATLICLDHIQEQISQYSPDNLQSELTPSNLANVIYTSGSTGKP KGVMVEHRGLVNLASSQIQSFAVKNNSRVLQFASFSFDACISEI LMTFGSGATLYLAQKNDLLPGQPLMERLEKNKITHVTLPPSALA VLPKKPLPNLQTLIVAGEACPLDLVKQWSVGRNFFNAYGPTETS VCATIGQCYQDDLKVTIGKAIANVQIYILDAFLQPVPIGVPGEL YIGGVGVARGYLNRPELTAERFIPNPFDPPLTPLKKGGDKSYET FKKGEEQPSKLYKTGDLARYLPDGNIEYLGRIDNQVKIRGFRIE LGEIEAVLSQCPDVQNTAV SEQ ID LQLAQIWSEILGINNIGIQENFFELGGHSLLAVSLINRIEQKLD NO. 18 KRLPLTSLFQNGTIASLAQLL T4 SEQ ID TPFFAVHPIGGNVLCYADLARNLGTKQPFYGLQSLGLSELEKTV NO. 19 ASIEEMAMIYIEAIQTVQASGPYYLGGWSMGGVIAFEIAQQLLT TE QGQEVALLALIDSYSPSLLNSVNREKNSANSLTEEFNEDINIAY SFIRDLASIFNQEISFSGSELAHFTSDELLDKFITWSQETNLLP SDFGKQQVKTWFKVFQINHQALSSYSPKTYLGRSVFLGAEDSSI KNPGWHQ SEQ ID FSLYYFGSYEAEFNPNKYNLLFEGAKFGDRAGFTALWIPERHFH NO. 20 AFGGFSPNPSVLAAALARETKQIQLRSGSVVLPLHNSIRVAEEW MO AVVDNLSQGRVGIAFASGWHPQDFVLAYQSFGQHRELMFQEIET VQKLWRGEAITVPDGKGQRVEVKTYPQPMQSQLPSWITIVNNPD TYIRAGAIGANILTNLMGQSVEDLARNIALYRQSLAEHGYDPAS GTVTVLLHTFVGKDLEQVREQARQPFGQYLTSSVGLLQNMVKSQ GMKVDFEQLRDEDRDFLLASAYKRYTETSALIGTPESCRQIIDH LQSIGVDEVACFIDFGVDEQTVLANLPYLQSLKDLYQ SEQ ID IDPPLTPLDKGIDPPLTPLDKGIDPPLTPLDKG NO. 21 SP 1 SEQ ID PYQGGLGGDQSPYQGGLGGDQSPYQGGLGGDQSPYQGGLGGDQS NO. 22 PYQGGLGGDQSPYQGELGGDQSPYQGGLGGDQV SP 2 SEQ ID PASEMREWVENTVSRILAFQPERGLEIGCGTGLLLSRVAKHCLE NO. 23 YWATDYSQGAIQYVERVCNAVEGLEQVKLRCQMADNFEGIALHQ MT FDTVVLNSIIQYFPSVDYLLQVLEGAINVIGERGQIFVGDVRSL PLLEPYHAAVQLAQASDSKTVEQWQQQVRQSVAGEEELVIDPTL FLALKQHFPQISWVEIQPKRGVAHNELTQFRYDVTLHLETINNQ ALLSGNPTVITWLNWQLDQLSLTQIKDKLLTDKPELWGIRGIPN QRVEEALKIWEWVENAPDVETVEQLKKLLKQQVDTGINPEQVWQ LAESLGYTAHLSWWESSQDGSFDVIFQRNSEAEDSKKLTLSKLA FWDEKPFKIKPWSDYTNNPLRGKLVQKLIP SEQ ID MTNYGKSMSHYYDLVVGHKGYNKDYATEVEFIHNLVETYTTEAK NO. 24 SILYLGCGTGYHAALLAQKGYSVHGVDLSAEMLEQAKTRIEDET MT 2 IASNLSFSQGNICEIRLNRQFNVVLALFHVVNYQTTNQNLLATF ATVKNHLKAGGIFICDVSYGSYVLGEFKSRPTASILRLEDNSNG NEVTYISELNFLTHENIVEVTHNLWVTNQENQLLENSRETHLQR YLFKPEVELLADACELTVLDAMPWLEQRPLTNIPCPSVCFVIGH KTTHSA SEQ ID ATGACTATTAACTATGGTGATCTGCAAGAACCCTTTAATAAATT NO. 25 CTCAACCCTAGTTGAATTACTCCGTTATCGGGCAAGCAGTCAAC A* CGGAACGCCTCGCCTATATTTTTCTGCGAGACGGAGAAATCGAA nucl GAAGCTCGTTTAACCTATGGGGAACTGGATCAAAAGGCTAGGGC acid GATC GCCGCTTATCTACAATCCTTAGAAGCCGAGGGCGAAAGGGGTTT ACTGCTCTATCCCCCAGGACTAGATTTTATTTCAGCTTTTTTTG GTTGTTTATATGCGGGAGTCGTTGCCATTCCCGCCTATCCACCC CGACGGAATCAAAACCTTTTGCGTTTACAGGCGATTATTGCCGA TTCTCAAGCCCGATTTACCTTCACCAATGCCGCTCTATTTCCCA GTTTAAAAAACCAATGGGCTAAAGACCCTGAATTAGGAGCAATG GAATGGATTGTTACCGATGAAATTGACCATCACCTCAGGGAGGA TTGGCTAGAACCAACCCTCGAAAAAAACAGTCTCGCTTTTCTAC AATACACCTCTGGTTCAACGGGAACTCCAAAGGGAGTAATGGTC AGTCACCATAATTTGTTGATTAATTCAGCCGATTTAGATCGTGG TTGGGGCCATGATCAAGATAGCGTAATGGTCACTTGGCTACCGA CCTTCCATGATATGGGTCTGATTTATGGGGTTATTCAGCCTTTG TACAAAGGATTTCTTTGTTACATGATGTCCCCTGCCAGCTTTAT GGAACGACCGTTACGTTGGTTACAGGCCCTTTCTGATAAAAAAG CAACCCATAGTGCGGCCCCCAACTTTGCCTACGATCTTTGTGTG CGGAAAATTCCCCCTGAAAAACGGGCTAGGTTAGACTTAAGCCA TTGGTGCATGGCCTTAAATGGGGCCGAACCCGTCAGAGCGGAGG TACTTAAAAAGTTTGCGGAGGCTTTTCAAGTTTCTGGTTTCAAA GCCACAGCCCTTTGTCCTGGCTACGGTTTAGCAGAAGCCACCCT GAAAGTTACGGCGGTTAGTTATGACAGTCCCCCTTACTTTTATC CCGTTCAGGCTAATGCTTTAGAAAAAAATAAGATTGTGGGAGCC ACTGAAACCGATACCAATGTGCAGACCCTCGTGGGC TGCGGCTGGACAACGATTGATACTCAAATCGTCATTGTCAATCC TGAAACCCTGAAACCTTGCTCCCCTGAAATTGTCGGCGAAATTT GGGTATCAGGTTCAACAATCGCCCAAGGCTATTGGGGAAAACCT CAAGAGACTCAGGAAACCTTTCAAGCTTATTTGGCAGATACAGG AGCC GGGCCTTTTCTGCGAACAGGAGACTTGGGCTTCATTAAAGATGG TGAATTGTTTATCACAGGTCGGCTCAAGGAAATTATTCTGATTC GAGGACGCAATAATTATCCCCAGGATATTGAATTAACCGTCCAA AATAGTCATCCCGCTCTGCGTCCCAGTTGTGGGGCTGCTTTTAC CGTTGAAAATAAGGGCGAAGAAAAGCTCGTGGTCGTTCAGGAAG TGGAGCGCACCTGGCTCCGT AAGGTAGATATAGATGAGGTAAAAAGAGCCATTCGTAAAGCTGT TGTCCAGGAATATGAT TTACAGGTTTATGCGATCGCGCTGATCAGGACTGGCAGTTTACC AAAAACCTCTAGCGGTAAAATTCAGCGTCGTAGCTGTCGGGCCA AATTTTTAGAGGGAAGCCTGGAAATTTTGGGCTAA SEQ ID ATGTCCACAGAAATCCCAAACGACAAAAAACAACCGACCCTAAC NO. 26 GAAAATTCAAAACTGG ACP TTAGTGGCTTACATGACAGAGATGATGGAAGTGGACGAAGATGA nucl GATTGATCTGAGCGTTCCCTTTGATGAATATGGTCTCGATTCTT acid CTATGGCAGTTGCTTTGATCGCTGATCTAGAGGATTGGTTACGA CGAGATTTACATCGCACCCTGATCTACGATTATCCAACTCTAGA AAAGTTGGCTAAACAGGTTAGTGAACCCTGA SEQ ID ATGGAACCCATCGCAATTATTGGTCTTGCTTGCCGCTTTCCAGG NO. 27 GGCTGACAATCCAGAAGCTTTCTGGCAACTCATGCGAAATGGGG KS TGGATGCGATCGCCGATATTCCTCCTGAACGTTGGGATATTGAG nucl CGTTTCTACGATCCCACACCTGCCACTGCCAAGAAGATGTATAG acid TCGCCAGGGCGGTTTTCTAAAAAATGTCGATCAATTTGACCCTC AATTTTTCCGAATTTCTCCCCTAGAAGCCACCTATCTAGATCCT CAACAAAGACTGCTACTGGAAGTCACCTGGGAAGCCTTAGAAAA TGCTGCCATTGTGCCTGAAACCTTAGCTGGTAGCCAATCAGGGG TTTTTATTGGTATCAGTGATGTGGATTATCATCGTTTGGCTTAT CAAAGTCCTACTAACTTGACCGCCTATGTGGGTACAGGCAACAG CACCAGTATTGCGGCTAACCGTTTATCATATCTGTTTGATTTGC GTGGCCCCAGTTTGGCCGTAGATACCGCTTGCTCTTCTTCCCTC GTCGCCGTTCACTTGGCCTGTCAGAGTTTGCAAAGTCAAGAATC GAACCTCTGCTTAGTGGGGGGAGTTAATCTCATTTTGTCGCCAG AGACAACCGTTGTTTTTTCCCAAGCGAGAATGATCGCCCCCGAC AGTCGTTGTAAAACCTTTGACGCGAGGGCCGATGGTTATGTGCG CTCGGAAGGCTGTGGAGTAGTCGTACTTAAACGTCTTAGGGATG CCATTCAGGACGGCGATCGCATTTTAGCAGTGATTGAAGGTTCC GCGGTGAATCAGGATGGTTTAAGTAATGGACTCACGGCCCCTAA TGGCCCTGCTCAACAGGCGGTGATTCGTCAGGCCCTGGCAAATG CCCAGGTAAAACCGGCCCAG ATTAGCTATGTCGAAGCCCATGGCACGGGGACAGAATTGGGGGA TCCGATCGAAGTTAAA TCTCTGAAAGCGGTTTTGGGTGAAAAGCGATCGCTCGATCAAAC CTGTTGGCTCGGTTCTGTGAAAACCAACATTGGTCATTTAGAAG CGGCGGCGGGAATGGCGGGTCTGATTAAAGTC GTTCTCTGCCTACAACACCAAGAAATTCCCCCTAATCTCCACTT TCAAACCCTTAATCCCTATATTTCCCTAGCTGACACAGCTTTTG CGATTCCCACTCAGGCTCAACCCTGGCGGACCAAACCCCCTAAG TCTGGTGAAAACGGTGTCGAACGACGTTTAGCAGGACTCAGTTC CTTTGGGTTTGGGGGGACAAATTCCCATGTGATTCTC SEQ ID GTTTTTCTATTTGCCGGTCAAGGTTCTCAATATGTAGGTATGGG NO. 28 TCGTCAACTGTACGAAACCCAACCCATCTTTCGCCAAACCTTGG AT ATCGCTGTGCTGAAATCCTGCGACCCCATTTAGATCAACCCCTC nucl TTAGAAATTCTTTATCCTGCTGACCCAGAAGCCGAAACAGCGAG acid TTTTTACCTAGAGCAGACTGCCTATACCCAACCCACTTTATTCG CATTCGAGTATGCCCTAGCACAGTTATGGCGTTCCTGGGGAATA GAACCGGCGGCAGTAATTGGTCACAGTGTCGGTGAATATGTGGC GGCCACCGTTGCCGGAGCCTTAAGTCTAGAAGAAGGATTAACGC TAATTGCCAAACGGGCAAAACTGATGCAGTCTCTCCCCAAGAAT GGGACAATGATGGCCGTTTTTGCCGCAGAAGAGCGGGTTAAAGC TGTTATTGAGCCTTATAGGACTGATGTAGCGATCGCTGCTGTTA ATGGACCAGAAAATTTTGTTATTTCAGGAAAAGCGCCGATTATT GCTGAGATTATCATTCATTTAACGGCAGCAGGAATAGAAGTTCG TCCTCTCAAAGTTTCCCATGCTTTTCACTCGCACCTGTTGGAGC CAATTTTAGATTCCTTAGAACAGGAAGCTGCTGCTATTTCCTAC CAACCCCTGCAAATTCCCTTAGTTGCTAATTTAACGGGGGAAGT TCTACCAGAAGGAGCAACGATTGAGGCTCGTTACTGGCGAAATC ATGCACGCAACCCTGTACAATTTTATGGGAGTATCCAAACGCTG ATCGAGCAGAAATTCAGTCTTTTTTTAGAAGTTAGCCCTAAACC GACTTTATCTCGATTGGGTCAACAATGTTGTCCAGAAAGATCGA CCACTTGGCTATTTTCCCTCGCCCCTCCTCAAGAAGAAGAACAA AGCCTACTAAATAGTTTGGCGATTCTCTATGATTCCCAAGGAGC CGAA SEQ ID ATCACATTGCAAACCCTAGTGGGAAATTTACTGCAATTGTCCCC NO. 29 TGCTGATGTCAATGTTCATACACCTTTCCTGGAGATGGGGGCAG ACP 2 ATTCCATTGTCATGGTTGAGGCGGTCAGACGGATTGAGAATACC nucl TATAACGTTAAAATTGCTATGCGTCAGTTATTTGAGGAGTTATC acid TACTTTAGATGCTTTAGCTACTTATTTA SEQ ID AAAGAGATGCTTTATCCCATTGTGGCCCAACGTTCTCAAGGATC NO. 30 AAGAATTTGGGATGTGGACGGTAATGAATATATTGATATGACGA AMT TGGGGCAAGGGGTAACGCTGTTTGGGCATCAA nucl CCAGACTTCATTATGTCGGCCCTACAAAGCCAACTCACTGAAGG acid CATTCATCTCAATCCGCGATCGCCAATTGTGGGAGAAGTGGCCG CCTTAATTTGTGAACTAACAGGAGCCGAACGA GCTTGTTTTTGCAACTCTGGAACCGAAGCCGTAATGGCCGCTAT TCGTATCGCCAGGGCAACAACAGGTCGGAGTAAAATTGCCCTCT TTGAAGGCTCCTATCATGGACATGCGGACGGAACCCTTTTTAGG AACCAAATTATTGATAACCAACTCCACTCTTTTCCCCTAGCTCT AGGCGTTCCCCCCAGCCTTAGTTCCGATGTGGTGGTATTGGACT ATGGCAGTGCGGAAGCTCTGAACTATTTACAAACCCAGGGGCAG GATTTAGCGGCGGTCTTAGTAGAACCAATTCAAAGTGGCAATCC TCTACTCCAACCCCAACAATTTCTCCAAAGTCTGCGACAAATTA CCAGTCAAATGGGCATTGCCCTGATTTTTGATGAAATGATTACG GGTTTTCGATCGCACCCAGGGGGAGCGCAAGCTTTATTTGGAGT ACAGGCGGATATTGCCACCTATGGCAAAGTAGTTGCGGGAGGAA TGCCCATTGGAGTTATTGCAGGTAAGGCCCATTATCTGGACAGC ATTGACGGGGGAATGTGGCGTTATGGCGATAAATCCTATCCTGG GGTGGACAGAACCTTTTTTGGGGGAACCTTTAATCAGCATCCGT TAGCAATGGTAGCGGCTAGGGCTGTCCTGACCCATTTAAAGGAG CAGGGGCCAGGTCTGCAACAACAATTAACTGAACGCACTGCGGC CTTAGCCGATACACTG AATCATTATTTTCAAGCCGAAGAAGTTCCTATTAAAATCGAACA GTTTAGTTCTTTCTTCCGGTTTGCCCTCTCTGGCAATTTGGATT TACTTTTCTATCACATGGTAGAAAAAGGTATTTATGTCTGGGAA TGGCGTAAACATTTTCTTTCAACCGCCCATACGGAAGCCGATCT TGCCCAATTTGTCCAAGCGGTTAAGGATAGCATCACAGAATTGC GT SEQ ID GGGGGGGATCAAGTCCCTCTCACCGAAGCCCAACGACAACTGTG NO. 31 GATTTTGGCTCAATTAGGAGACAACGGCTCTGTGGCCTATAACC C nucl AATCAGTGACATTGCAATTAAGTGGCCCATTAAATCCCGTCGCA acid ATGAATCAAGCTATTCAACAAATCAGCGATCGCCATGAAGCGTT ACGAACCAAAATTAATGCCCAGGGAGATAGTCAAGAAATCCTGC CCCAGGTCGAAATTAACTGC CCTATCTTAGACTTCAGTCTTGACCAAGCTTCGGCCCAACAGCA AGCAGAACAATGGTTAAAGGAAGAAAGTGAAAAACCCTTTGATT TGAGCCAGGGTTCTCTCGTGCGTTGGCATCTACTCAAATTAGAA CCAGAATTACATTTGTTAGTATTAACGGCCCATCACATTATCAG TGACGGTTGGTCAATGGGGGTAATCCTTCGGGAATTAGGAGAGT TATATTCAGCCAAATGTCAGGGTGTTACGGCTAATCTTAAAACC CCAAAACAGTTTCGAGAATTGATTGAATGGCAAAGCCAGCCAAG CCAAGGGGAAGAACTGAAAAAACAGCAAGCCTATTGGTTAGCAA CCCTTGCC GATCCCCCTGTTTTGAATTTACCCACTGACAAACCTCGTCCAGC TTTACCCAGTTACCAAGCTAATCGTCGAAGTCTAACTTTAGATA GCCAATTTACAGAAAAACTAAAGCAATTTAGTCGTAAACAGGGC TGTACCTTGCTGATGACCCTGTTATCGGTTTATAACATTCTCGT TCATCGTTTGACGGGACAGGATGATATTCTGGTGGGTCTGCCAG CCTCTGGACGGGGGCTTTTAGATAGTGAAGGTATGGTGGGTTAT TGCACCCATTTTTTACCAATTCGCAGTCAATTAGCA SEQ ID ACTTACAGTGAATTAAATTGTCGAGCCAATCAGTTAGCACATTA NO. 32 TTTACAAAAATTAGGAGTTGGGCCAGAGGTCTTAGTCGGTATTT A nucl TGGTCGAACGTTCTTTAGAAATGATTGTCGGATTGTTAGGGATT acid CTCAAGGCTGGGGGAGCCTATGTACCTCTTGATCCTGACTATCC CCCTGAACGTCTTCAATTTATGTTAGAAGATAGTCAATTTTTTC TCCTCTTAACCCAACAGCATTTACTGGAATCTTTTGCTCAGTCT TCAGAAACGGCTACTCCCAAGATTATTTGTTTGGATAGCGACTA CCAAATTATTTCCCAGGCAAAGAATATTAATCCCGAAAATTCAG TCACAACGAGTAATCTTGCCTATGTAATTTATACCTCTGGTTCG ACAGGTAAACCGAAGGGCGTGATGAATAATCATGTTGCTATTAG TAATAAATTGTTATGGGTACAAGACACTTATCCTCTAACCACAG AAGACTGTATTTTACAAAAAACTCCCTTTAGTTTTGATGTTTCA GTGTGGGAATTATTCTGGCCCCTACTAAACGGAGCGCGTTTGGT TTTTGCCAAGCCGAATGGCCATAAAGATGCCAGTTACTTAGTCA ATCTGATTCAAGAGCAACAAGTAACAACGCTACATTTTGTGTCT TCTATGCTACAGCTTTTTCTGACAGAAAAAGACGTAGAAAAATG TAATAGTCTTAAACGAGTCATTTGTAGTGGTGAAGCCCTTTCTT TAGAGCTTCAAGAACGTTTTTTTGCTCGTTTAGTCTGTGAATTA CACAATCTTTATGGACCGACAGAAGCCGCTATTCATGTCACATT TTGGCAATGTCAATCAGATAGCAATTTGAAAACAGTACCCATTG GTCGGCCGATCGCTAATATCCAAATTTACATTTTAGACTCTCAT TTCAGCCAGTACCTATTGGAGTAATCGGAGAATTGCACATTGGT GGGGTTGGTTTGGCGCGGGGTTATTTAAACAGGCCTGAGTTAAC GGCGGAGAAATTTATTGCAAATCCGTTTGCTTCCCTTGATCCCC CCCTAACCCCCCTTGATAAGGGGGGAGATGAGAGCTATAAAACT TTTAAAAAGGGGGGAGAGCAACCATCAAGATTGTATAAA ACGGGAGATTTAGCTCGTTATTTACCCGATGGCAAGATTGAGTA TCTAGGGCGCATTGATAATCAGGTAAAAATTCGCGGTTTCCGGA TTGAATTGGGGGAAATTGAAGCGGTTTTGCTATCCCATCCCCAG GTACGAGAAGCGGTCGTT SEQ ID GAGGCGATCGCCGCTATTTTTGGTCAAGTTTTAAAACTGGAAAA NO. 33 AGTGGGAATTTATGATAACTTTTTTGAGATCGGCGGTAATTCTT T nucl TGCAAGCCACTCAAGTTATTTCACGCTTACGAGAAAGTTTTGCC acid CTAGAGTTGCCCTTGCGTCGCCTGTTTGAACAACCGACTGTGGC GGATTTGGCTTTAGCCGTA SEQ ID CCTCGTGATGGCCAATTACCCCTCTCCTTTGCCCAGTCGCGACT NO. 34 CTGGTTCTTGTATCAATTAGAAGGAGCCACGGGAACCTATAACA C2 TGACAGGGGCCTTGAGTTTAAGCGGGCCTCTTCAGGTCGAAGCC nucl CTCAAACAAGCCCTAAGAACTATCATTCAACGCCATGAGCCATT acid GCGTACCAGTTTCCAATCGGTTGACGGGGTTCCAGTGCAGGTGA TTAATCCCTATCCTGTTTGGGAATTAGCGATGGTTGATTTGACA GGAAAGGAGACAGAAGCAGAAAAATTGGCCTATCAG GAATCCCAAACCCCGTTTGATTTGACCAATAGTCCTTTGTTGAG GGTAACGCTCCTCAAATTACAGCCAGAAAAGCATATTTTATTAA TTAATATGCACCATATTATTTCCGATGGCTGGTCAATCGGTGTT TTTGTTCGTGAATTGTCCCATCTCTATAGGGCTTTTGTGGCGGG TAAAGAACCAACTTTACCGATTTTACCAATTCAGTATGCGGATT TTGCCGTTTGGCAGCGAGAGTGGTTACAGGGTAAGGTTTTAGCG GCTCAATTGGAATATTGGAAGCGACAATTGGCAGATGCTCCTCC TCTGCTGGAACTGCCCACTGATCGCCCTCGTCCCGCAATCCAAA CCTTTCAAGGCAAGACAGAAAGATTTGAGCTAGATAGGAAACTG ACCCAAGAATTAAAGGCATTAAGT CAACAGTCGGGTTGTACTTTATTTATGACTTTGTTGGCCGCTTT TGGGGTGGTTTTATCCCGTTATAGTGGCCAGACTGATATCGTCA TTGGTTCGGCGATCGCCAACCGTAATCGCCAAGACATTGAGGGG TTAATTGGCTTTTTTGTTAACACTTTGGCGTTGAGGTTAGATTT ATCA SEQ ID ACCTATGGAGAATTAAACCATCGCGCCAATCAATTAGCTCACTA NO. 35 TCTTCAGTCGTTAGGAGTCACCAAAGAACAAATCGTCGGGGTTT A2 ATCTGGAACGTTCCCTTGAAATGGCGATCGGATTTTTAGGTATT nucl CTCAAAGCAGGAGCCGCCTATCTCCCCATTGATCCTGAATATCC acid CTCAGTACGCACCCAATTTATTCTCGAAGATACCCAACTTTCGC TTCTCTTAACTCAGGCAGAACTGGCAGAAAAACTGCCCCAGACT CAAAACAAAATTATCTGTCTAGATCGGGACTGGCCA GAAATTACCTCCCAACCCCAGACAAACCTAGACCTAAAGATAGA ACCTAATAACCTAGCC TATTGCATCTATACTTCTGGTTCCACAGGACAACCCAAAGGAGT ACTGATTTCCCATCAAGCCCTACTCAACTTAATTTTCTGGCATC AACAAGCGTTTGAGATTGGCCCCTTACATAAAGCGACCCAAGTG GCAGGCATTGCTTTCGATGCAACGGTTTGGGAATTGTGGCCCTA TCTGACCACAGGAGCCTGTATTAATCTGGTTCCCCAAAATATTC TGCTCTCACCGACGGATTTACGGGATTGGTTGCTTAACCGAGAA ATTACCATGAGTTTTGTGCCAACTCCTTTAGCTGAAAAATTATT ATCCTTGGATTGGCCTAACCATTCTTGTCTAAAAACCCTGTTAC TGGGAGGTGACAAACTTCATTTTTATCCTGCTGCGTCCCTTCCC TTTCAGGTCATTAACAACTATGGCCCAACGGAAAATACAGTGGT TGCGACCTCTGGACTGGTCAAATCATCTTCATCTCATCACTTTG GAACTCCGACTATTGGTCGTCCCATTGCCAACGTCCAAATCTAT TTATTAGACCAAAACCTACAACCTGTCCCCATTGGTGTACCAGG AGAATTACATTTAGGTGGGGCGGGTTTAGCGCAGGGCTATCTCA ATCGTCCTGAGTTAACGGCTGAAAAATTTATTGCCAATCCCTTT GATCCCCCCCTAACCCCCCTTGATAAGGGGGGAGAAGAACCCTC AAAACTCTATAAAACG GGAGACTTAGCCCGTTATTTACCCGATGGCAATGTAGAATTTTT GGGACGTATTGACAATCAGGTAAAAATTCGGGGTTTTCGCATCG AAACTGGGGAAATCGAAGCCGTTTTAAGTCAATATTTCCTATTA GCTGAAAGTGTAGTC SEQ ID GCTCAACTGACTCAAATTTGGAGTGAAGTTTTGGGACTGGAACG NO. 36 CATTGGCGTTAAGGACAACTTTTTTGAATTGGGAGGACATTCTC T2 TTTTGGCTACCCAGGTTTTATCAAGAATTAATTCAGCCTTTGGA nucl CTTGATCTTTCTGTGCAAATTATGTTTGAATCACCAACGATCGC acid GGGCATTGCGGGTTATATT SEQ ID GCTAGAGACGGTCATTTACCCCTGTCTTTTGCTCAACAACGTTT NO. 37 ATGGTTTTTACATTATCTTTCCCCTGATAGTCGTTCCTACAATA C3 CCCTGGAAATATTGCAAATTGATGGGAATCTCAATCTGACTGTG nucl CTAGAGCAGAGTTTGGGGGAATTAATTAACCGCCATGAAATTTT acid TAGAACAACATTCCCCACTGTTTCAGGGGAACCGATTCAGAAAA TTGCACTTCCTAGTCGTTTTCAGTTAAAAGTTGATAATTATCAA GATTTAGACGAAAATGAACAATCAGCTAAAATTCAACAAGTAGC AGAATTGGAAGCAGGACAAGCTTTTGATTTAACGGTGGGGCCAC TGATTCAGTTTAAGCTATTGCAATTGAGTCCCCAGAAGTCGGTG CTGCTGTTGAAAATGCACCATATTATCTATGATGGCTGGTCTTT TGGGATTCTGATTCGGGAATTATCGGCTCTATACGAAGCATTTT TAAAGAACTTAGCCAATCCTCTCCCTGCGTTGTCTATTCAGTAT GCAGATTTTGCGGTTTGGCAACGTCAATATCTCTCAGGTGAGGT CTTAGATAAACAACTCAATTATTGGCAAGAACAGTTAGCAACAG TCTCTCCTGTTCTTACTTTACCAACGGATAGACCCCGTCCGGCG ATACAAACTTTTCAGGGAGGAGTTGAGCGTTTTCAACTGGATCA AAATGTCACTCAAGGTCTTAAAAAGTTAGGTCAAGATCAGGTTG CAACCCTGTTTATGACGTTGTTGGCCGGTTTCGGCGTTTTGCTA TCTCGTTATAGTGGTCAATCTGATCTGATGGTGGGTTCTCCGAT CGCTAATCGTAATCAAGCAGCGATCGAACCTTTAATTGGCTTTT TTGCTAACACTTTGGCTTTAAGAATTAATTTATCA SEQ ID ACATACACTGAATTAAACCATCGCGCTAATCAGTTAGCCCATTA NO. 38 TTTACAAACTTTAGGCGTGGGAGCAGAAGTCTTAGTCGGTATTT A3 CCCTAGAACGTTCTTTAGAGATGATTATCGGCTTATTAGGGATT nucl CTCAAGGTAGGTGGTGCTTATCTTCCTCTTGATCCAGACTATCC acid CACTGAGCGTCTTCAGTTGATGTTAGAAGACAGTCAAGTTCCTT TTTTGATTACCCACAGTTCTTTATTAGCAAAATTGCCTCCCTCT CAAGCAACTCTGATTTGTTTAGATCATATCCAAGAGCAGATTTC TCAATATTCTCCAGATAATCTTCAATGTCAGTTAACTCCTGCCA ATTTAGCTAACGTTATTTATACCTCTGGCTCTACGGGTAAGCCT AAAGGGGTGATGGTTGAACATAAAGGTTTAGTTAACTTAGCTCT TGCTCAAATTCAATCTTTTGCAGTCAACCATAACAGTCGTGTGC TGCAATTTGCTTCTTTTAGTTTTGATGCTTGTATTTCAGAAATT TTGATGACCTTTGGTTCTGGAGCGACGCTTTATCTTGCACAAAA AGATGCTTTATTGCCAGGTCAGCCATTAATTGAACGGTTAGTAA AGAATGGAATTACTCATGTGACTTTGCCGCCTTCAGCTTTAGTG GTTTTACCCCAGGAACCGTTACGCAACTTAGAAACCTTAATTGT GGCGGGTGAGGCTTGTTCTCTTGATTTAGTGAAACAATGGTCAA TCGATAGAAACTTTTTCAATGCCTATGGGCCAACGGAAGCGAGT GTTTGTGCCACTATTGGACAATGTTATCAAGATGATTTAAAGGT GACGATTGGTAAGGCGATCGCCAATGTCCAAATTTATATTTTAG ATGCCTTTTTACAGCCGGTGCCGGTGGGAGTGTCAGGAGAGTTA TACATTGGTGGAGTTGGGGTGGCAAGGGGCTATTTAAATCGTCC TGAATTAACCCAAGAAAAATTTATTGCTAATCCTTTTAGTAACG ACCCAGATTCTCGGCTCTATAAAACTGGCGACTTAGCGCGTTAT TTACCCGATGGTAATATTGAATATTTAGGACGCATTGACAATCA GGTAAAAATTCGCGGTTTTCGCATTGAGTTAGGAGAAATTGAAG CGGTTCTGAGTCAATGTCCCGATGTGCAAAATACGGCGGTG SEQ ID GAAATTCTGGCTCAAATATGGGGGCAAGTTCTCAAGATAGAAAG NO. 39 AGTCAGCAGAGAAGAT T3 AATTTCTTTGAATTGGGGGGGCATTCCCTTTTAGCTACCCAGGT nucl AATGTCCCGTCTGCGTGAAACTTTTCAAGTCGAATTACCTTTGC acid GTAGTCTCTTTACCGCTCCCACTATTGCTGAATTGGCCCTAACA ATT SEQ ID AACGACAGTGCTAACCTCCCGTTATCTTTTGCTCAACAACGTTT NO. 40 ATGGTTTCTGGATCAATTAGAACCTAACAGCGCCTTTTATCATG C4 TAGGGGGAGCCGTAAGACTAGAAGGAACATTAAATATTACTGCC nucl TTAGAGCAAAGCTTAAAAGAAATTATTAATCGTCATGAAGCTTT acid ACGCACAAATTTTATAACGATTGATGGTCAAGCCACTCAAATTA TTCACCCTACTATTAATTGGCGATTGTCTGTTGTTGATTGTCAA AATTTAACCGACACTCAATCTCTGGAAATTGCGGAAGCTGAAAA GCCCTTTAATCTTGCTCAAGATTGCTTATTTCGTGCTACTTTAT TCGTGCGATCACCGCTAGAATATCATCTACTCGTGACCATGCAC CATATTGTTAGCGATGGCTGGTCAATTGGAGTATTTTTTCAAGA ACTAACTCATCTTTACGCTGTCTATAATCAGGGTTTACCCTCAT CTTTAACGCCTATTAAAATACAATATGCTGATTTTGCGGTCTGG CAACGGAATTGGTTACAAGGTGAAATTTTAAGTAATCAATTGAA TTATTGGCGCGAACAATTAGCAAATGCTCCTGCTTTTTTACCTT TACCGACAGATAGACCTAGGCCCGCAATCCAAACTTTTATTGGT TCTCATCAAGAATTTAAACTTTCTCAGCCATTAAGCCAAAAATT GAATCAACTAAGTCAGAAGCATGGAGTGACTTTATTTATGACTC TCCTGGCTGCTTTTGCTACCTTACTTTACCGTTATACAGGACAA GCAGATATTTTAGTTGGTTCTCCTATTGCTAACCGTAATCGTAA GGAAATTGAGGGATTAATCGGCTTTTTTGTTAATACATTAGTTC TGAGATTGAGTTTAGAT SEQ ID ACCTATGCTGAATTAAATCATCAAGCTAATCAGTTAGTCCATTA NO. 41 CTTACAAACTTTAGGAATTGGGCCAGAGGTCTTAGTCGCTATTT A4 CAGTAGAACGTTCTTTAGAAATGATTATCGGCTTATTAGCCATT nucl CTCAAGGCGTGTGGTGCTTATCTCCCTCTTGCTCCTGACTATCC acid CACTGAGCGTCTTCAGTTCATGTTAGAAGATAGTCAAGCTTCTT TTTTGATTACCCACAGTTCTTTATTAGAAAAATTGCCTTCTTCT CAAGCGACTCTAATTTGTTTAGATCACATCCAAGAGCAGATTTC TCAATATTCTCCCGATAATCTTCAAAGTGAGTTAACTCCTTCCA ATTTGGCTAACGTTATTTACACCTCTGGCTCTACGGGTAAGCCT AAAGGGGTGATGGTTGAACATCGGGGCTTAGTTAACTTAGCGAG TTCTCAAATTCAATCTTTTGCAGTCAAAAATAACAGTCGTGTAC TGCAATTTGCTTCCTTTAGTTTTGATGCTTGTATTTCAGAAATT TTGATGACCTTTGGTTCTGGAGCGACTCTTTATCTTGCTCAAAA AAATGATTTATTGCCAGGTCAGCCATTAATGGAAAGGTTAGAAA AGAATAAAATTACCCATGTTACTTTACCCCCTTCAGCTTTAGCT GTTTTACCAAAAAAACCGTTACCCAACTTACAAACTTTAATTGT GGCGGGTGAGGCTTGTCCTCTGGATTTAGTCAAACAATGGTCAG TCGGTAGAAACTTTTTCAATGCCTATGGCCCGACAGAAACGAGT GTTTGTGCCACGATTGGACAATGTTATCAAGATGATTTAAAGGT CACGATTGGTAAGGCGATCGCTAATGTCCAAATTTATATTTTGG ATGCCTTTTTACAACCAGTACCCATCGGAGTACCAGGGGAATTA TACATTGGTGGAGTCGGAGTTGCGAGGGGTTATCTAAATCGTCC TGAATTAACGGCGGAAAGATTTATTCCTAATCCTTTTGATCCCC CCCTAACCCCCCTTAAAAAGGGGGGAGATAAGAGCTATGAAACT TTTAAAAAGGGGGAAGAGCAACCA TCAAAACTCTATAAAACGGGAGATTTAGCTCGTTATTTACCCGA TGGCAATATTGAATATTTAGGACGCATTGACAATCAGGTAAAAA TTCGCGGTTTTCGCATTGAGTTAGGAGAAATTGAAGCGGTTCTG AGTCAATGTCCCGATGTGCAAAATACGGCGGTG SEQ ID TTACAATTAGCTCAAATCTGGTCAGAGATTTTAGGCATTAATAA NO. 42 TATTGGTATTCAGGAAAACTTCTTTGAATTAGGCGGTCATTCTT T4 TATTAGCAGTCAGTCTGATCAATCGTATTGAACAAAAGTTAGAT nucl AAACGTTTACCATTAACCAGTCTTTTTCAAAATGGAACCATAGC acid AAGTCTAGCTCAATTACTAG SEQ ID ACTCCATTTTTTGCTGTTCATCCCATTGGTGGTAATGTGCTATG NO. 43 TTATGCCGATTTAGCTCGTAATTTAGGAACGAAACAGCCGTTTT TE ATGGATTACAATCATTAGGGCTAAGTGAATTAGAAAAAACTGTA nucl GCCTCTATTGAAGAAATGGCGATGATTTATATTGAAGCAATACA acid AACTGTTCAAGCCTCTGGTCCCTACTATTTAGGAGGTTGGTCAA TGGGAGGAGTGATAGCTTTTGAAATCGCCCAACAATTATTGACC CAAGGTCAAGAAGTTGCTTTACTGGCTTTAATAGATAGTTATTC TCCCAGTTTACTTAATTCAGTTAATAGGGAGAAAAATTCTGCTA ATTCCCTGACAGAAGAATTTAATGAAGATATCAATATTGCCTAT TCTTTCATCAGAGACTTAGCAAGTATATTTAATCAAGAAATCTC TTTCTCTGGGAGTGAACTTGCTCATTTTACATCAGACGAATTAC TAGACAAGTTTATTACTTGGAGTCAAGAGACGAATCTTTTGCCG TCAGATTTTGGGAAGCAGCAGGTTAAAACCTGGTTTAAAGTTTT CCAGATTAATCACCAAGCTTTGAGCAGCTATTCTCCCAAGACGT ATCTGGGTAGAAGTGTTTTCTTAGGAGCGGAAGACAGTTCTATT AAAAATCCTGGTTGGCATCAA SEQ ID AGCGGGTCTCAAGACCAAAAAACGATACAGTTTAGCCTCTACTA NO. 44 CTTTGGTAGCTATGAAGCGGAATTTAACCCGAATAAATATAACT MO TACTGTTTGAAGGAGCTAAATTTGGCGATCGCGCTGGTTTTACG nucl GCCCTTTGGATTCCTGAACGTCATTTCCACGCTTTTGGTGGTTT acid TTCTCCCAATCCTTCGGTTTTGGCGGCGGCTTTAGCACGGGAAA CCAAACAGATTCAACTGCGATCAGGCAGTGTGGTTTTACCGCTA CATAATTCCATCCGAGTCGCCGAAGAATGGGCAGTGGTGGACAA TCTTTCCCAGGGCCGCGTTGGTATTGCTTTTGCATCGGGTTGGC ATCCCCAGGATTTTGTCTTGGCTCCCCAGTCCTTTGGCCAACAT CGGGAATTGATGTTCCAAGAAATTGAAACCGTCCAGAAACTTTG GCGAGGGGAAGCGATCACCGTGCCAGACGGAAAGGGTCAA AGGGTAGAGGTTAAAACCTATCCCCAACCGATGCAGTCCCAGTT ACCCAGCTGGATTACTATTGTCAATAATCCCGATACCTATATCA GAGCAGGGGCGATCGGTGCTAATATCCTTACCAATCTGATGGGG CAAAGCGTGGAAGATTTAGCCCGTAATATTGCGCTATATCGTCA ATCTTTGGCAGAGCATGGTTATGATCCCGCGTCGGGAACGGTGA CAGTTCTCCTGCATACTTTTGTTGGCAAGGATTTAGAACAAGTT CGAGAACAGGCTCGCCAACCCTTTGGGCAATACCTCACCTCCTC TGTCGGACTCTTGCAGAACATGGTCAAGAGCCAGGGCATGAAAG TGGATTTTGAACAATTAAGAGACGAAGATCGGGACTTTCTCCTC GCTTCTGCCTATAAACGCTATACAGAAACCAGTGCTTTAATTGG CACACCCGAATCCTGTCGTCAAATTATTGATCATTTGCAGTCCA TCGGTGTGGATGAAGTGGCTTGTTTTATTGATTTTGGGGTAGAT GAACAAACAGTTTTGGCCAATTTACCCTATCTCCAGTCCCTAAA AGACTTATATCAA SEQ ID ATTGATCCCCCCCTAACCCCCCTTGATAAGGGGATTGATCCCCC NO. 45 CCTAACCCCCCTTGATAAGGGGATTGATCCCCCCCTAACCCCCC SP 1 TTGATAAGGGG nucl acid SEQ ID CCTTATCAAGGGGGGTTAGGGGGGGATCAATCCCCTTATCAAGG NO. 46 GGGGTTAGGGGGGGAT SP 2 CAATCCCCTTATCAAGGGGGGTTAGGGGGTGATCAATCCCCTTA nucl TCAAGGGGGGTTAGGGGGTGATCAATCCCCTTATCAAGGGGGGT acid TAGGGGGGGATCAATCCCCTTATCAAGGAGAG TTAGGGGGGGATCAATCCCCTTATCAAGGGGGGTTAGGGGGGGA TCAAGTC SEQ ID CCTGCTTCAGAAATGCGAGAGTGGGTCGAAAACACTGTTAGTCG NO. 47 CATCTTGGCTTTCCAACCAGAACGCGGTTTAGAAATTGGTTGTG MT GTACAGGTTTGTTACTCTCCAGGGTAGCAAAGCATTGTCTTGAA nucl TATTGGGCAACGGATTATTCCCAAGGGGCGATCCAGTATGTTGA acid ACGGGTTTGCAATGCCGTTGAAGGTTTAGAACAGGTTAAATTAC GCTGTCAAATGGCAGATAATTTTGAAGGTATTGCCCTACATCAA TTTGATACCGTCGTCTTAAATTCGATTATTCAGTATTTTCCCAG TGTGGATTATCTGTTACAGGTGCTTGAAGGGGCGATCAACGTCA TTGGCGAGCGAGGTCAGATTTTTGTCGGGGATGTGCGGAGTTTA CCCCTATTAGAGCCATATCATGCGGCTGTGCAATTAGCCCAAGC TTCTGACTCGAAAACTGTTGAACAATGGCAACAACAGGTGCGTC AAAGTGTAGCAGGTGAAGAAGAACTGGTCATTGATCCCACATTG TTCCTGGCTTTAAAACAACATTTTCCGCAAATTAGCTGGGTAGA AATTCAACCGAAACGGGGTGTGGCTCACAATGAGTTAACTCAAT TTCGCTATGATGTCACTCTCCATTTAGAGACTATCAATAATCAA GCATTATTGAGCGGCAATCCAACGGTAATTACCTGGTTAAATTG GCAACTTGACCAACTGTCTTTAACACAAATTAAAGATAAATTAT TAACAGACAAACCTGAATTGTGGGGAATTCGTGGTATTCCTAAT CAGCGAGTTGAAGAGGCTCTAAAAATTTGGGAATGGGTGGAAAA TGCCCCTGATGTTGAAACGGTTGAACAACTCAAAAAACTTCTCA AACAACAAGTAGATACTGGTATTAATCCTGAACAGGTTTGGCAA TTAGCTGAGTCTCTCGGTTACACCGCTCACCTTAGTTGGTGGGA AAGTAGTCAAGACGGTTCCTTTGATGTCATTTTTCAGCGGAATT CAGAAGCGGAGGACTCAAAAAAATTAACCCTTTCAAAACTTGCT TTCTGGGATGAAAAACCCTTTAAAATAAAGCCCTGGAGTGACTA TACTAACAACCCTCTGCGCGGTAAGTTAGTCCAAAAATTAATTC CT SEQ ID ATGACAAATTATGGCAAATCTATGTCTCATTACTATGATCTAGT NO. 48 GGTAGGACATAAAGGTTATAACAAAGATTACGCCACTGAAGTAG MT 2 AATTCATTCACAATTTAGTTGAGACTTACACAACTGAAGCCAAA nucl TCTATCCTATACTTGGGCTGTGGTACGGGTTATCATGCCGCTCT acid TTTAGCACAGAAAGGGTATTCTGTACATGGTGTTGATCTCAGTG CTGAAATGTTAGAGCAGGCTAAAACTCGCATTGAAGATGAAACA ATAGCTTCTAATCTGAGTTTTTCTCAAGGAAATATTTGTGAAAT CCGTTTAAATCGTCAGTTTAATGTTGTTCTTGCTCTATTTCATG TGGTTAACTATCAAACGACCAATCAAAATTTACTGGCAACGTTT GCAACGGTTAAAAACCATTTAAAAGCTGGGGGGATTTTTATTTG TGATGTGTCCTATGGGTCTTACGTACTGGGGGAATTTAAGAGTC GGCCTACGGCATCAATATTGCGTTTAGAGGATAATTCCAATGGT AACGAAGTAACCTATATTAGTGAACTAAATTTTTTAACCCATGA AAATATAGTGGAAGTTACTCACAATTTATGGGTAACAAATCAAG AAAATCAACTTCTAGAGAATTCACGGGAAACACATCTTCAGCGC TATCTTTTCAAGCCTGAAGTTGAATTGTTGGCTGATGCTTGTGA ACTAACTGTTCTTGATGCGATGCCCTGGCTTGAACAACGTCCTT TGACAAACATTCCTTGTCCTTCAGTTTGTTTTGTTATTGGGCAT AAAACAACCCATTCAGCTTAA SEQ ID CCGACCTGTGATAAACAATTC NO. 49 Primer A SEQ ID CKNCCDGTDATRAANARYTC NO. 50 Primer B SEQ ID TTCAATATCCTGGGGATA NO. 51 Primer C SEQ ID YTCDATRTCYTGNGGRTA NO. 52 Primer D SEQ ID CGTTGGTTACAGGCCCTTTCT NO. 53 Primer E SEQ ID MGNTGGYTNCARGCNYTNWS NO. 54 Primer F SEQ ID TTAGACTTAAGCCATTGG NO. 55 Primer G SEQ ID YTNGAYYTNWSNCAYTGG NO. 56 Primer H SEQ ID CATAGAAGAATCGAGACCATATTC NO. 57 Primer I SEQ ID CATNSWNSWRTCNARNCCRTAYTC NO. 58 Primer J SEQ ID MTTQTASSANALASFNQFLRDVKAIAQPYWYPTVSNKRSFSEVI NO. 59 RSWGMLSLLIFLIVGLVAVTAFNSFVNRRLIDVIIQEKDASQFA ABC STLTVYAIGLICVTLLAGFTKDIRKKIALDWYQWLNTQIVEKYF Trans- SNRAYYKINFQSDIDNPDQRLAQEIEPIATNAISFSATFLEKSL porter EMLTFLVVVWSISRQIAIPLMFYTIIGNFIAAYLNQELSKINQA QLQSKADYNYALTHVRTHAESIAFFRGEKEEQNIIQRRFQEVIN DTKNKINWEKGNEIFSRGYRSVIQFFPFLVLGPLYIKGEIDYGQ VEQASLASFMFASALGELITEFGTSGRFSSYVERLNEFSNALET VTKQAENVSTITTIEENHFAFEHVTLETPDYEKVIVEDLSLTVQ KGEGLLIVGPSGRGKSSLLRAIAGLWNAGTGRLVRPPLEEILFL PQRPYIILGTLREQLLYPLTNSEMSNTELQAVLQQVNLQNVLNR VDDFDSEKPWENILSLGEQQRLAFARLLVNSPSFTILDEATSAL DLTNEGILYEQLQTRKTTFISVGHRESLFNYHQWVLELSADSSW ELLSVQDYRLKKAGEMFTNASSNNSITPDITIDNGSEPEIVYSL EGFSHQEMKLLTDLSLSSIRSKASRGKVITAKDGFTYLYDKNPQ ILKWLR SEQ ID ATGACAACCCAAACAGCTTCTAGTGCCAATGCCCTTGCTTCCTT NO. 60 TAACCAATTTTTAAGGGATGTAAAGGCGATCGCCCAACCCTATT ABC GGTATCCCACTGTATCAAATAAAAGAAGCTTTTCTGAGGTTATT Trans- CGTTCCTGGGGAATGCTATCACTGCTTATCTTTTTGATTGTGGG porter ATTAGTCGCCGTCACGGCTTTTAATAGTTTTGTTAATCGTCGTT Nucl TAATTGATGTCATTATTCAAGAAAAAGATGCGTCTCAATTTGCC acid AGTACATTAACTGTCTATGCGATCGGATTAATCTGTGTAACGCT GCTGGCAGGGTTCACTAAAGATATTCGCAAAAAAATTGCCCTAG ATTGGTATCAATGGTTAAACACCCAGATTGTAGAGAAATATTTT AGTAATCGTGCCTATTATAAAATTAACTTTCAATCTGACATTGA TAACCCCGATCAACGTCTAGCCCAGGAAATTGAACCGATCGCCA CAAACGCCATTAGTTTCTCGGCCACTTTTTTGGAAAAAAGTTTG GAAATGCTAACTTTTTTAGTGGTAGTTTGGTCAATTTCTCGACA GATTGCTATTCCGCTAATGTTTTACACGATTATCGGTAATTTTA TTGCCGCCTATCTAAATCAAGAATTAAGCAAGATCAATCAGGCA CAACTGCAATCAAAAGCAGATTATAACTATGCCTTAACCCATGT TCGGACTCATGCGGAATCTATTGCTTTTTTTCGGGGAGAAAAAG AGGAACAAAATATTATTCAGCGACGTTTTCAGGAAGTTATCAAT GATACGAAAAATAAAATTAACTGGGAAAAAGGGAATGAAATTTT TAGT CGGGGCTATCGTTCCGTCATTCAGTTTTTTCCTTTTTTAGTCCT TGGCCCTTTGTATATTAAAGGAGAAATTGATTATGGACAAGTTG AGCAAGCTTCATTAGCTAGTTTTATGTTTGCATCGGCCCTGGGA GAATTAATTACAGAATTTGGTACTTCAGGACGTTTTTCTAGTTA TGTAGAACGTTTAAATGAATTTTCTAATGCCTTAGAAACTGTGA CTAAACAAGCCGAGAATGTCAGCACAATTACAACCATAGAAGAA AATCATTTTGCCTTTGAACACGTCACCCTAGAAACCCCTGACTA TGAAAAGGTGATTGTTGAGGATTTATCTCTTACTGTTCAAAAAG GTGAAGGATTATTGATTGTCGGGCCCAGTGGTCGAGGTAAAAGT TCTTTATTAAGGGCGATCGCCGGTTTATGGAATGCTGGCACTGG GCGTTTAGTGCGTCCTCCCCTAGAAGAAATTCTCTTTTTGCCCC AACGTCCCTACATTATTTTGGGAACCTTACGCGAACAATTGCTG TATCCTCTAACCAATAGTGAGATGAGCAATACCGAACTTCAAGC AGTATTACAACAAGTCAATTTGCAAAATGTGCTAAATCGGGTGG ATGACTTTGACTCCGAAAAACCCTGGGAAAACATTCTCTCCCTC GGTGAACAACAACGCCTAGCCTTTGCTCGATTGTTAGTGAATTC TCCGAGTTTTACCATTTTAGATGAGGCGACCAGTGCCTTAGATT TAACAAATGAGGGGATTTTATACGAGCAATTACAAACTCGCAAG ACAACCTTTATTAGTGTGGGTCATCGAGAAAGTTTGTTTAATTA CCATCAATGGGTTTTAGAACTTTCTGCTGACTCTAGTTGGGAAC TCTTAAGCGTTCAAGATTATCGCCTTAAAAAAGCGGGAGAAATG TTTACTAATGCTTCGAGTAACAATTCCATAACACCCGATATTAC TATCGATAATGGATCAGAACCAGAAATAGTCTATTCTCTTGAAG GATTTTCCCATCAGGAAATGAAACTATTAACAGACCTATCACTC TCTAGCATTCGGAGTAAAGCCAGTCGAGGGAAGGTGATTACAGC CAAGGATGGTTTTACCTACCTTTATGACAAAAATCCTCAGATAT TAAAGTGGCTCAGAACTTAA In one embodiment the entire gene cluster is transformed and expressed in a heterologous system. SEQ ID NO. 61 encompasses the genes of said cluster.

    1-27260 ATGACTATTAACTATGGTGATCTGCAAGAACCCTTTA Microginin- ATAAATTCTCAACCCTAGTTGAATTACTCCGTTATCG Cluster GGCAAGCAGTCAACCGGAACGCCTCGCCTATATTTTT     1-1743 CTGCGAGACGGAGAAATCGAAGAAGCTCGTTTAACCT Adenylation- ATGGGGAACTGGATCAAAAGGCTAGGGCGATCGCCGC Protein (A*) TTATCTACAATCCTTAGAAGCCGAGGGCGAAAGGGGT  1892-2158 TTACTGCTCTATCCCCCAGGACTAGATTTTATTTCAG Acyl-Carrier- CTTTTTTTGGTTGTTTATATGCGGGAGTCGTTGCCAT Protein (ACP) TCCCGCCTATCCACCCCGACGGAATCAAAACCTTTTG  2204-3016 CGTTTACAGGCGATTATTGCCGATTCTCAAGCCCGAT Methyltrans- TTACCTTCACCAATGCCGCTCTATTTCCCAGTTTAAA ferase (MT) AAACCAATGGGCTAAAGACCCTGAATTAGGAGCAATG  3464-13123 GAATGGATTGTTACCGATGAAATTGACCATCACCTCA PKS/NRPS (KS- GGGAGGATTGGCTAGAACCAACCCTCGAAAAAAACAG AT-ACP-AMT- TCTCGCTTTTCTACAATACACCTCTGGTTCAACGGGA MO-C-A-T) ACTCCAAAGGGAGTAATGGTCAGTCACCATAATTTGT 13120-17832 TGATTAATTCAGCCGATTTAGATCGTGGTTGGGGCCA NRPS 2 (C-A- TGATCAAGATAGCGTAATGGTCACTTGGCTACCGACC Mt-T) TTCCATGATATGGGTCTGATTTATGGGGTTATTCAGC 17836-25194 CTTTGTACAAAGGATTTCTTTGTTACATGATGTCCCC NRPS 3 (C-A- TGCCAGCTTTATGGAACGACCGTTACGTTGGTTACAG T-C-A-T) GCCCTTTCTGATAAAAAAGCAACCCATAGTGCGGCCC 25257-27260 CCAACTTTGCCTACGATCTTTGTGTGCGGAAAATTCC ABC- CCCTGAAAAACGGGCTACGTTAGACTTAAGCCATTGG Transporter TGCATGGCCTTAAATGGGGCCGAACCCGTCAGAGCGG (ABC) AGGTACTTAAAAAGTTTGCGGAGGCTTTTCAAGTTTC TGGTTTCAAAGCCACAGCCCTTTGTCCTGGCTACGGT TTAGCAGAAGCCACCCTGAAAGTTACGGCGGTTAGTT ATGACAGTCCCCCTTACTTTTATCCCGTTCAGGCTAA TGCTTTAGAAAAAAATAAGATTGTGGGAGCCACTGAA ACCGATACCAATGTGCAGACCCTCGTGGGCTGCGGCT GGACAACGATTGATACTCAAATCGTCATTGTCAATCC TGAAACCCTGAAACCTTGCTCCCCTGAAATTGTCGGC GAAATTTGGGTATCAGGTTCAACAATCGCCCAAGGCT ATTGGGGAAAACCTCAAGAGACTCAGGAAACCTTTCA AGCTTATTTGGCAGATACAGGAGCCGGGCCTTTTCTG CGAACAGGAGACTTGGGCTTCATTAAAGATGGTGAAT TGTTTATCACAGGTCGGCTCAAGGAAATTATTCTGAT TCGAGGACGCAATAATTATCCCCAGGATATTGAATTA ACCGTCCAAAATAGTCATCCCGCTCTGCGTCCCAGTT GTGGGGCTGCTTTTACCGTTGAAAATAAGGGCGAAGA AAAGCTCGTGGTCGTTCAGGAAGTGGAGCGCACCTGG CTCCGTAAGGTAGATATAGATGAGGTAAAAAGAGCCA TTCGTAAAGCTGTTGTCCAGGAATATGATTTACAGGT TTATGCGATCGCGCTGATCAGGACTGGCAGTTTACCA AAAACCTCTAGCGGTAAAATTCAGCGTCGTAGCTGTC GGGCCAAATTTTTAGAGGGAAGCCTGGAAATTTTGGG CTAAGAAAATTTCTCGATCGGCACTTAATGTGTTAAA TTCGTATGTCGATTGAAACTTCGACCAATTCTTTCTC TCCCCTTAAGTCCATGTCTCTGGATTTGAAAATTCCT TAAACTTTAACTACATTTCTCAAGAAAGCAAATTGAA TCTAATGTCCACAGAAATCCCAAACGACAAAAAACAA CCGACCCTAACGAAAATTCAAAACTGGTTAGTGGCTT ACATGACAGAGATGATGGAAGTGGACGAAGATGAGAT TGATCTGAGCGTTCCCTTTGATGAATATGGTCTCGAT TCTTCTATGGCAGTTGCTTTGATCGCTGATCTAGAGG ATTGGTTACGACGAGATTTACATCGCACCCTGATCTA CGATTATCCAACTCTAGAAAAGTTGGCTAAACAGGTT AGTGAACCCTGACATTTTTATAAAGTTTGTGCTTAAA AATTTTGAGGAAGTTCTAAAATGACAAATTATGGCAA ATCTATGTCTCATTACTATGATCTAGTGGTAGGACAT AAAGGTTATAACAAAGATTACGCCACTGAAGTAGAAT TCATTCACAATTTAGTTGAGACTTACACAACTGAAGC CAAATCTATCCTATACTTGGGCTGTGGTACGGGTTAT CATGCCGCTCTTTTAGCACAGAAAGGGTATTCTGTAC ATGGTGTTGATCTCAGTGCTGAAATGTTAGAGCAGGC TAAAACTCGCATTGAAGATGAAACAATAGCTTCTAAT CTGAGTTTTTCTCAAGGAAATATTTGTGAAATCCGTT TAAATCGTCAGTTTAATGTTGTTCTTGCTCTATTTCA TGTGGTTAACTATCAAACGACCAATCAAAATTTACTG GCAACGTTTGCAACGGTTAAAAACCATTTAAAAGCTG GGGGGATTTTTATTTGTGATGTGTCCTATGGGTCTTA CGTACTGGGGGAATTTAAGAGTCGGCCTACGGCATCA ATATTGCGTTTAGAGGATAATTCCAATGGTAACGAAG TAACCTATATTAGTGAACTAAATTTTTTAACCCATGA AAATATAGTGGAAGTTACTCACAATTTATGGGTAACA AATCAAGAAAATCAACTTCTAGAGAATTCACGGGAAA CACATCTTCAGCGCTATCTTTTCAAGCCTGAAGTTGA ATTGTTGGCTGATGCTTGTGAACTAACTGTTCTTGAT GCGATGCCCTGGCTTGAACAACGTCCTTTGACAAACA TTCCTTGTCCTTCAGTTTGTTTTGTTATTGGGCATAA AACAACCCATTCAGCTTAAATTCTGCTAAAAAAAATC CAACTTACCTTATTCTCTGAAACCACACAAGCCATGA ATACAATTCAAGATGCCAAGACCGAAAATTACTCAAT CTTAAATCAGTCAATTCCAAGACCTCTCAAACTGAGT AATATCCTATTACGATAAGATTTTGCGTTCTCCTTTG TTTGGAATGTCAGCAGAGGAGTCTCTATATTGGCTAG AGAAATGTTTATGTCAAGAGCATCAGGGCTTCGATGT ACAAGTTAAGTATCATCAAAAAATGCTGAAGAATATG TTACGTTTGACCGATAGTTTGGATTATCTATGGCCAG TTAACCGTGAAATGCGGCTCATGAAAGCTGGGGGGTC AATTGAACGGGCGATCACCAATAACATTAAAGCTTTT CTTCAATTTAAAGAAACTGTAACCGTATTAAATTAGA AAAACCGCAGTGAGGAATTTGAATGGAACCCATCGCA ATTATTGGTCTTGCTTGCCGCTTTCCAGGGGCTGACA ATCCAGAAGCTTTCTGGCAACTCATGCGAAATGGGGT GGATGCGATCGCCGATATTCCTCCTGAACGTTGGGAT ATTGAGCGTTTCTACGATCCCACACCTGCCACTGCCA AGAAGATGTATAGTCGCCAGGGCGGTTTTCTAAAAAA TGTCGATCAATTTGACCCTCAATTTTTCCGAATTTCT CCCCTAGAAGCCACCTATCTAGATCCTCAACAAAGAC TGCTACTGGAAGTCACCTGGGAAGCCTTAGAAAATGC TGCCATTGTGCCTGAAACCTTAGCTGGTAGCCAATCA GGGGTTTTTATTGGTATCAGTGATGTGGATTATCATC GTTTGGCTTATCAAAGTCCTACTAACTTGACCGCCTA TGTGGGTACAGGCAACAGCACCAGTATTGCGGCTAAC CGTTTATCATATCTGTTTGATTTGCGTGGCCCCAGTT TGGCCGTAGATACCGCTTGCTCTTCTTCCCTCGTCGC CGTTCACTTGGCCTGTCAGAGTTTGCAAAGTCAAGAA TCGAACCTCTGCTTAGTGGGGGGAGTTAATCTCATTT TGTCGCCAGAGACAACCGTTGTTTTTTCCCAAGCGAG AATGATCGCCCCCGACAGTCGTTGTAAAACCTTTGAC GCGAGGGCCGATGGTTATGTGCGCTCGGAAGGCTGTG GAGTAGTCGTACTTAAACGTCTTAGGGATGCCATTCA GGACGGCGATCGCATTTTAGCAGTGATTGAAGGTTCC GCGGTGAATCAGGATGGTTTAAGTAATGGACTCACGG CCCCTAATGGCCCTGCTCAACAGGCGGTGATTCGTCA GGCCCTGGCAAATGCCCAGGTAAAACCGGCCCAGATT AGCTATGTCGAAGCCCATGGCACGGGGACAGAATTGG GGGATCCGATCGAAGTTAAATCTCTGAAAGCGGTTTT GGGTGAAAAGCGATCGCTCGATCAAACCTGTTGGCTC GGTTCTGTGAAAACCAACATTGGTCATTTAGAAGCGG CGGCGGGAATGGCGGGTCTGATTAAAGTCGTTCTCTG CCTACAACACCAAGAAATTCCCCCTAATCTCCACTTT CAAACCCTTAATCCCTATATTTCCCTAGCTGACACAG CTTTTGCGATTCCCACTCAGGCTCAACCCTGGCGGAC CAAACCCCCTAAGTCTGGTGAAAACGGTGTCGAACGA CGTTTAGCAGGACTCAGTTCCTTTGGGTTTGGGGGGA CAAATTCCCATGTGATTCTCAGCGAAGCCCCTGTCAC CGTTAAAAACAATCAACAAAATGGGCAGAAGTTGATA GAACGTCCCTGGCATTTGCTGACTTTATCTGCCAAGA ATGAAGAAGCCTTAAAAGCCTTAGTCCATTGTTATCA AAAGTATTTAGCTGATCATCATGAAATTCCTCTCGCT GATGTTTGTTTTACGGCCAATAGTCGGCGATCGCACT TTAATCATCGTTTAGGAGTAGTGGCTAGAGATCGCTT AGAAATGTTGCAGAAGTTAGAGAACTTTAGTAACCAA GAAAGGATGAGAGAACCGAAGAGTATTAACAAAAAAG AAAAACCTAAAATTGTTTTTCTATTTGCCGGTCAAGG TTCTCAATATGTAGGTATGGGTCGTCAACTGTACGAA ACCCAACCCATCTTTCGCCAAACCTTGGATCGCTGTG CTGAAATCCTGCGACCCCATTTAGATCAACCCCTCTT AGAAATTCTTTATCCTGCTGACCCAGAAGCCGAAACA GCGAGTTTTTACCTAGAGCAGACTGCCTATACCCAAC CCACTTTATTCGCATTCGAGTATGCCCTAGCACAGTT ATGGCGTTCCTGGGGAATAGAACCGGCGGCAGTAATT GGTCACAGTGTCGGTGAATATGTGGCGGCCACCGTTG CCGGAGCCTTAAGTCTAGAAGAAGGATTAACGCTAAT TGCCAAACGGGCAAAACTGATGCAGTCTCTCCCCAAG AATGGGACAATGATCGCCGTTTTTGCCGCAGAAGAGC GGGTTAAAGCTGTTATTGAGCCTTATAGGACTGATGT AGCGATCGCTGCTGTTAATGGACCAGAAAATTTTGTT ATTTCAGGAAAAGCGCCGATTATTGCTGAGATTATCA TTCATTTAACGGCAGCAGGAATAGAAGTTCGTCCTCT CAAAGTTTCCCATGCTTTTCACTCGCACCTGTTGGAG CCAATTTTAGATTCCTTAGAACAGGAAGCTGCTGCTA TTTCCTACCAACCCCTGCAAATTCCCTTAGTTGCTAA TTTAACGGGGGAAGTTCTACCAGAAGGAGCAACGATT GAGGCTCGTTACTGGCGAAATCATGCACGCAACCCTG TACAATTTTATGGGAGTATCCAAACGCTGATCGAGCA GAAATTCAGTCTTTTTTTAGAAGTTAGCCCTAAACCG ACTTTATCTCGATTGGGTCAACAATGTTGTCCAGAAA GATCGACCACTTGGCTATTTTCCCTCGCCCCTCCTCA AGAAGAAGAACAAAGCCTACTAAATAGTTTGGCGATT CTCTATGATTCCCAAGGAGCCGAAATAAACTGGGAAG GGTTTAATCAAAATTATCCCCACCATTTACTGGCTCT ACCGACCTATCCTTTTCAACGTCAACGCTATTGGCTT GAAACCGGTAAACCGACTTCTGAAGAAACAACCATGA CGACCAATGCCACTAATGTCCAAGCTATCTCCAGCCA TCAAAAACAACAGGAGATTCTAATCACATTGCAAACC CTAGTGGGAAATTTACTGCAATTGTCCCCTGCTGATG TCAATGTTCATACACCTTTCCTGGAGATGGGGGCAGA TTCCATTGTCATGGTTGAGGCGGTCAGACGGATTGAG AATACCTATAACGTTAAAATTGCTATGCGTCAGTTAT TTGAGGAGTTATCTACTTTAGATGCTTTAGCTACTTA TTTAGCTCAAAATCCGGCTACTGATTGCCAAACTGCT CAAATTAATACCGAGGTGTTTTCTGCGCCCATTGCCT GCTCAAATAACCGATCGCCCAATGTCGTGCTGAGTTC TAATACCAACGGCTTTCAACGTCAAACAGCTTCTCCA GGTTTTTCGGCGATCGCCCCCCTTGCAGGAATGGGAG GAGCAGGGGAAATGGGAGGAGTTGAAGTGCCTCAAGT TTCTGTGCCACAAACCAGTGCGGTAACAGCCTCAGGT TCAACCGTTTCTAGTTCTGCCCTGGAAAACATTATGG GTCAACAGTTACAACTGATGGCCAAACAGTTAGAAGT CTTGCAAACGGCCAATTTTGCCCCGACGACTCCCCGA ACCACAGAAAATTCCCCATCTTCCGTCAGTCAAAATA GGTCAAACGGACTTACACAACAGTTAATTCCCCCCCA GCAATTAGCGGCGAACCTAGAGCCAATAGCCAGTCGC ACCCGTCAAACCAGCAATCAAGCTTCTGCTCCTAAAC CGACAGTAACAGCCACTCCCTGGGGGCCGAAAAAACC ACCCACAGGTGGATTCACTCCCCAACAACAGCAACAT CTAGAGGCATTAATTGCTCGCTTTACGGAACGTACCA AAACCTCTAAGCAAATTGTGCAAAGCGATCGCCTGCG TTTAGCAGATAGTCGAGCCTCGGTCGGATTCCGTATG TCTATTAAAGAGATGCTTTATCCCATTGTGGCCCAAC GTTCTCAAGGATCAAGAATTTGGGATGTGGACGGTAA TGAATATATTGATATGACGATGGGGCAAGGGGTAACG CTGTTTGGGCATCAACCAGACTTCATTATGTCGGCCC TACAAAGCCAACTCACTGAAGGCATTCATCTCAATCC GCGATCGCCAATTGTGGGAGAAGTGGCCGCCTTAATT TGTGAACTAACAGGAGCCGAACGAGCTTGTTTTTGCA ACTCTGGAACCGAAGCCGTAATGGCCGCTATTCGTAT CGCCAGGGCAACAACAGGTCGGAGTAAAATTGCCCTC TTTGAAGGCTCCTATCATGGACATGCGGACGGAACCC TTTTTAGGAACCAAATTATTGATAACCAACTCCACTC TTTTCCCCTAGCTCTAGGCGTTCCCCCCAGCCTTAGT TCCGATGTGGTGGTATTGGACTATGGCAGTGCGGAAG CTCTGAACTATTTACAAACCCAGGGGCAGGATTTAGC GGCGGTCTTAGTAGAACCAATTCAAAGTGGCAATCCT CTACTCCAACCCCAACAATTTCTCCAAAGTCTGCGAC AAATTACCAGTCAAATGGGCATTGCCCTGATTTTTGA TGAAATGATTACGGGTTTTCGATCGCACCCAGGGGGA GCGCAAGCTTTATTTGGAGTACAGGCGGATATTGCCA CCTATGGCAAAGTAGTTGCGGGAGGAATGCCCATTGG AGTTATTGCAGGTAAGGCCCATTATCTGGACAGCATT GACGGGGGAATGTGGCGTTATGGCGATAAATCCTATC CTGGGGTGGACAGAACCTTTTTTGGGGGAACCTTTAA TCAGCATCCGTTAGCAATGGTAGCGGCTAGGGCTGTC CTGACCCATTTAAAGGAGCAGGGGCCAGGTCTGCAAC AACAATTAACTGAACGCACTGCGGCCTTAGCCGATAC ACTGAATCATTATTTTCAAGCCGAAGAAGTTCCTATT AAAATCGAACAGTTTAGTTCTTTCTTCCGGTTTGCCC TCTCTGGCAATTTGGATTTACTTTTCTATCACATGGT AGAAAAAGGTATTTATGTCTGGGAATGGCGTAAACAT TTTCTTTCAACCGCCCATACGGAAGCCGATCTTGCCC AATTTGTCCAAGCGGTTAAGGATAGCATCACAGAATT GCGTCAGGGAGGTTTTATCCCCGCAAAAAAGCCTTCC TGGCCAGTGCCAACGCCTCAAATTGATCCCCCCCTAA CCCCCCTTGATAAGGGGATTGATCCCCCCCTAACCCC CCTTGATAAGGGGATTGATCCCCCCCTAACCCCCCTT GATAAGGGGGGAGATGTTGATGTCGCGCTTGATAAGG GAGGAAATTCTCATTCTGTTAGGGACAGTAAGTTAGG GAAAGGGAGCGGGTCTCAAGACCAAAAAACGATACAG TTTAGCCTCTACTACTTTGGTAGCTATGAAGCGGAAT TTAACCCGAATAAATATAACTTACTGTTTGAAGGAGC TAAATTTGGCGATCGCGCTGGTTTTACGGCCCTTTGG ATTCCTGAACGTCATTTCCACGCTTTTGGTGGTTTTT CTCCCAATCCTTCGGTTTTGGCGGCGGCTTTAGCACG GGAAACCAAACAGATTCAACTGCGATCAGGCAGTGTG GTTTTACCGCTACATAATTCCATCCGAGTCGCCGAAG AATGGGCAGTGGTGGACAATCTTTCCCAGGGCCGCGT TGGTATTGCTTTTGCATCGGGTTGGCATCCCCAGGAT TTTGTCTTGGCTCCCCAGTCCTTTGGCCAACATCGGG AATTGATGTTCCAAGAAATTGAAACCGTCCAGAAACT TTGGCGAGGGGAAGCGATCACCGTGCCAGACGGAAAG GGTCAAAGGGTAGAGGTTAAAACCTATCCCCAACCGA TGCAGTCCCAGTTACCCAGCTGGATTACTATTGTCAA TAATCCCGATACCTATATCAGAGCAGGGGCGATCGGT GCTAATATCCTTACCAATCTGATGGGGCAAAGCGTGG AAGATTTAGCCCGTAATATTGCGCTATATCGTCAATC TTTGGCAGAGCATGGTTATGATCCCGCGTCGGGAACG GTGACAGTTCTCCTGCATACTTTTGTTGGCAAGGATT TAGAACAAGTTCGAGAACAGGCTCGCCAACCCTTTGG GCAATACCTCACCTCCTCTGTCGGACTCTTGCAGAAC ATGGTCAAGAGCCAGGGCATGAAAGTGGATTTTGAAC AATTAAGAGACGAAGATCGGGACTTTCTCCTCGCTTC TGCCTATAAACGCTATACAGAAACCAGTGCTTTAATT GGCACACCCGAATCCTGTCGTCAAATTATTGATCATT TGCAGTCCATCGGTGTGGATGAAGTGGCTTGTTTTAT TGATTTTGGGGTAGATGAACAAACAGTTTTGGCCAAT TTACCCTATCTCCAGTCCCTAAAAGACTTATATCAAC CTCATCTCCCCCCTTATCAAGGGGGGTTAGGGGGGGA TCAATCCCCTTATCAAGGGGGGTTAGGGGGGGATCAA TCCCCTTATCAAGGGGGGTTAGGGGGTGATCAATCCC CTTATCAAGGGGGGTTAGGGGGTGATCAATCCCCTTA TCAAGGGGGGTTAGGGGGGGATCAATCCCCTTATCAA GGAGAGTTAGGGGGGGATCAATCCCCTTATCAAGGGG GGTTAGGGGGGGATCAAGTCCCTCTCACCGAAGCCCA ACGACAACTGTGGATTTTGGCTCAATTAGGAGACAAC GGCTCTGTGGCCTATAACCAATCAGTGACATTGCAAT TAAGTGGCCCATTAAATCCCGTCGCAATGAATCAAGC TATTCAACAAATCAGCGATCGCCATGAAGCGTTACGA ACCAAAATTAATGCCCAGGGAGATAGTCAAGAAATCC TGCCCCAGGTCGAAATTAACTGCCCTATCTTAGACTT CAGTCTTGACCAAGCTTCGGCCCAACAGCAAGCAGAA CAATGGTTAAAGGAAGAAAGTGAAAAACCCTTTGATT TGAGCCAGGGTTCTCTCGTGCGTTGGCATCTACTCAA ATTAGAACCAGAATTACATTTGTTAGTATTAACGGCC CATCACATTATCAGTGACGGTTGGTCAATGGGGGTAA TCCTTCGGGAATTAGGAGAGTTATATTCAGCCAAATG TCAGGGTGTTACGGCTAATCTTAAAACCCCAAAACAG TTTCGAGAATTGATTGAATGGCAAAGCCAGCCAAGCC AAGGGGAAGAACTGAAAAAACAGCAAGCCTATTGGTT AGCAACCCTTGCCGATCCCCCTGTTTTGAATTTACCC ACTGACAAACCTCGTCCAGCTTTACCCAGTTACCAAG CTAATCGTCGAAGTCTAACTTTAGATAGCCAATTTAC AGAAAAACTAAAGCAATTTAGTCGTAAACAGGGCTGT ACCTTGCTGATGACCCTGTTATCGGTTTATAACATTC TCGTTCATCGTTTGACGGGACAGGATGATATTCTGGT GGGTCTGCCAGCCTCTGGACGGGGGCTTTTAGATAGT GAAGGTATGGTGGGTTATTGCACCCATTTTTTACCAA TTCGCAGTCAATTAGCAGGTAATCCCACTTTTGCTGA ATATCTCAAACAAATGCGGGGGGTTTTGTTGTCGGCT TATGAACATCAGGACTATCCCTTTGCTCTTTTGCTCA ATCAGTTAGATTTACCGCGTAATACCAGTCGCTCTCC TTTAATTGATGTCAGTTTCAATTTAGAACCAGTTATT AACCTACCCAAAATGAAAGGATTAGAGATTAGTTTGT TGCCTCAAAGTGTAAGTTTTAAGGATCGAGATTTGCA TTGGAATGTGACAGAAATGGGTGGAGAAGCTCTGATT GATTGTGACTACAATACAGACTTATTTAAAGATGAAA CGATTCAGCGTTGGTTAGGCCATTTTCAAACCTTACT TGAGGCAGTTATTAATGATTCGCAACAAAATCTGCGG GAATTACCCTTATTAAGTTCTGCTGAACGACAACAGT TATTAGTGGATTGGAATCAAACCAAGACCGACTATCC CCAAGATCAGTGTATTCATCAATTATTTGAAGCGCAA GTTGAACGGACTCCCGATGCGATTGCGGTGGTATTTG AAACTCAACAATTAACTTACAGTGAATTAAATTGTCG AGCCAATCAGTTAGCACATTATTTACAAAAATTAGGA GTTGGGCCAGAGGTCTTAGTCGGTATTTTGGTCGAAC GTTCTTTAGAAATGATTGTCGGATTGTTAGGGATTCT CAAGGCTGGGGGAGCCTATGTACCTCTTGATCCTGAC TATCCCCCTGAACGTCTTCAATTTATGTTAGAAGATA GTCAATTTTTTCTCCTCTTAACCCAACAGCATTTACT GGAATCTTTTGCTCAGTCTTCAGAAACGGCTACTCCC AAGATTATTTGTTTGGATAGCGACTACCAAATTATTT CCCAGGCAAAGAATATTAATCCCGAAAATTCAGTCAC AACGAGTAATCTTGCCTATGTAATTTATACCTCTGGT TCGACAGGTAAACCGAAGGGCGTGATGAATAATCATG TTGCTATTAGTAATAAATTGTTATGGGTACAAGACAC TTATCCTCTAACCACAGAAGACTGTATTTTACAAAAA ACTCCCTTTAGTTTTGATGTTTCAGTGTGGGAATTAT TCTGGCCCCTACTAAACGGAGCGCGTTTGGTTTTTGC CAAGCCGAATGGCCATAAAGATGCCAGTTACTTAGTC AATCTGATTCAAGAGCAACAAGTAACAACGCTACATT TTGTGTCTTCTATGCTACAGCTTTTTCTGACAGAAAA AGACGTAGAAAAATGTAATAGTCTTAAACGAGTCATT TGTAGTGGTGAAGCCCTTTCTTTAGAGCTTCAAGAAC GTTTTTTTGCTCGTTTAGTCTGTGAATTACACAATCT TTATGGACCGACAGAAGCCGCTATTCATGTCACATTT TGGCAATGTCAATCAGATAGCAATTTGAAAACAGTAC CCATTGGTCGGCCGATCGCTAATATCCAAATTTACAT TTTAGACTCTCATCTTCAGCCAGTACCTATTGGAGTA ATCGGAGAATTGCACATTGGTGGGGTTGGTTTGGCGC GGGGTTATTTAAACAGGCCTGAGTTAACGGCGGAGAA ATTTATTGCAAATCCGTTTGCTTCCCTTGATCCCCCC CTAACCCCCCTTGATAAGGGGGGAGATGAGAGCTATA AAACTTTTAAAAAGGGGGGAGAGCAACCATCAAGATT GTATAAAACGGGAGATTTAGCTCGTTATTTACCCGAT GGCAAGATTGAGTATCTAGGGCGCATTGATAATCAGG TAAAAATTCGCGGTTTCCGGATTGAATTGGGGGAAAT TGAAGCGGTTTTGCTATCCCATCCCCAGGTACGAGAA GCGGTCGTTTTGGTGAGCGAAAGCGATCGCTCTGAAA ATCGGGCTTTGGTCGCTTATATTGTCCCTAATGATCC TGCTTGTACGACTCAATCATTACGAGAGTTTGTTAAA CGGCAGCTTCCTGACTATATGATCCCAGCTTATTGGC TGATCCTTGACAATTTACCGTTAACCAGCAATGGCAA AATTGATCGTCGGGCTTTACCGTTACCTAATCCAGAG TTAAATCGTTCGATAGACTATGTGGCTCCCAAAAATC CTACCCAGGAGGCGATCGCCGCTATTTTTGGTCAAGT TTTAAAACTGGAAAAAGTGGGAATTTATGATAACTTT TTTGAGATCGGCGGTAATTCTTTGCAAGCCACTCAAG TTATTTCACGCTTACGAGAAAGTTTTGCCCTAGAGTT GCCCTTGCGTCGCCTGTTTGAACAACCGACTGTGGCG GATTTGGCTTTAGCCGTAACGGACATTCATGCCACTT TACAAAAATTACAAACCCCTATTGATGATTTATCAGG CGATCGCGAGGAGATTGAACTATGAAATCTATTGAAA CCTTTTTGTCAGATTTAGCCAATCAAGATATTAAACT CTGGATGGACGGCGATCGCCTGCGTTGTAATGCACCC CAGGGCCTATTAACCCCAGAGATTCAAACAGAACTGA AAAACCGTAAAGCAGAAATCATTCACTTTCTCAATCA ACTGGGTTCAGAGGAGCAAATTAATCCTAGAACGATT CTTCCCATTCCTCGTGATGGCCAATTACCCCTCTCCT TTGCCCAGTCGCGACTCTGGTTCTTGTATCAATTAGA AGGAGCCACGGGAACCTATAACATGACAGGGGCCTTG AGTTTAAGCGGGCCTCTTCAGGTCGAAGCCCTCAAAC AAGCCCTAAGAACTATCATTCAACGCCATGAGCCATT GCGTACCAGTTTCCAATCGGTTGACGGGGTTCCAGTG CAGGTGATTAATCCCTATCCTGTTTGGGAATTAGCGA TGGTTGATTTGACAGGAAGGAGACAGAAGCAGAAAAA ATTGGCCTATCAGGAATCCCAAACCCCGTTTGATTTG ACCAATAGTCCTTTGTTGAGGGTAACGCTCCTCAAAT TACAGCCAGAAAAGCATATTTTATTAATTAATATGCA CCATATTATTTCCGATGGCTGGTCAATCGGTGTTTTT GTTCGTGAATTGTCCCATCTCTATAGGGCTTTTGTGG CGGGTAAAGAACCAACTTTACCGATTTTACCAATTCA GTATGCGGATTTTGCCGTTTGGCAGCGAGAGTGGTTA CAGGGTAAGGTTTTAGCGGCTCAATTGGAATATTGGA AGCGACAATTGGCAGATGCTCCTCCTCTGCTGGAACT GCCCACTGATCGCCCTCGTCCCGCAATCCAAACCTTT CAAGGCAAGACAGAAAGATTTGAGCTAGATAGGAAAC TGACCCAAGAATTAAAGGCATTAAGTCAACAGTCGGG TTGTACTTTATTTATGACTTTGTTGGCCGCTTTTGGG GTGGTTTTATCCCGTTATAGTGGCCAGACTGATATCG TCATTGGTTCGGCGATCGCCAACCGTAATCGCCAAGA CATTGAGGGGTTAATTGGCTTTTTTGTTAACACTTTG GCGTTGAGGTTAGATTTATCAGAAAAACCCAGCTTTG CCGCTTTTTTAAAACAAGTACAGGAAGTCACTCAGGA TGCCTATGAGCATCAAGACTTGCCCTTTGAAATGTTA GTGGAAGAATTACAACTAGAGCGCAAATTAGACCGAA ATCCTTTGGTACAGGTGATGTTTGCCCTACAAAATGC GGCCAATGAAACCTGGAATTTACCTGGGTTGACCATT GAAGAAATGTCTTGGGAACTTGAACCTGCCCGTTTTG ACCTAGAGGTTCATTTATCAGAAGTTAACGCCGGCAT AGCTGGATTCTGTTGCTACACCATTGATCTATTTGAT GATGCAACGATCGCCCGTCTATTGGAACATTTTCAGA ATCTTCTCAGGGCAATTATTGTTAATCCTCAAGAATC GGTAAGTTTATTACCCTTGTTGTCAGAACAGGAAGAA AAGCAACTTTTAGTTGATTGGAATCAAACCCAAGCCG ATTATCCCCAAGATAAGCTTGTCCATCAGTTATTTGA AGTTCAAGCAGCCAGTCAGCCAGAAGCGATCGCTCTA ATCTTTGAAAATCAGGTTTTGACCTATGGAGAATTAA ACCATCGCGCCAATCAATTAGCTCACTATCTTCAGTC GTTAGGAGTCACCAAAGAACAAATCGTCGGGGTTTAT CTGGAACGTTCCCTTGAAATGGCGATCGGATTTTTAG GTATTCTCAAAGCAGGAGCCGCCTATCTCCCCATTGA TCCTGAATATCCCTCAGTACGCACCCAATTTATTCTC GAAGATACCCAACTTTCGCTTCTCTTAACTCAGGCAG AACTGGCAGAAAAACTGCCCCAGACTCAAAACAAAAT TATCTGTCTAGATCGGGACTGGCCAGAAATTACCTCC CAACCCCAGACAAACCTAGACCTAAAGATAGAACCTA ATAACCTAGCCTATTGCATCTATACTTCTGGTTCCAC AGGACAACCCAAAGGAGTACTGATTTCCCATCAAGCC CTACTCAACTTAATTTTCTGGCATCAACAAGCGTTTG AGATTGGCCCCTTACATAAAGCGACCCAAGTGGCAGG CATTGCTTTCGATGCAACGGTTTGGGAATTGTGGCCC TATCTGACCACAGGAGCCTGTATTAATCTGGTTCCCC AAAATATTCTGCTCTCACCGACGGATTTACGGGATTG GTTGCTTAACCGAGAAATTACCATGAGTTTTGTGCCA ACTCCTTTAGCTGAAAAATTATTATCCTTGGATTGGC CTAACCATTCTTGTCTAAAAACCCTGTTACTGGGAGG TGACAAACTTCATTTTTATCCTGCTGCGTCCCTTCCC TTTCAGGTCATTAACAACTATGGCCCAACGGAAAATA CAGTGGTTGCGACCTCTGGACTGGTCAAATCATCTTC ATCTCATCACTTTGGAACTCCGACTATTGGTCGTCCC ATTGCCAACGTCCAAATCTATTTATTAGACCAAAACC TACAACCTGTCCCCATTGGTGTACCAGGAGAATTACA TTTAGGTGGGGCGGGTTTAGCGCAGGGCTATCTCAAT CGTCCTGAGTTAACGGCTGAAAAATTTATTGCCAATC CCTTTGATCCCCCCCTAACCCCCCTTGATAAGGGGGG AGAAGAACCCTCAAAACTCTATAAAACGGGAGACTTA GCCCGTTATTTACCCGATGGCAATGTAGAATTTTTGG GACGTATTGACAATCAGGTAAAAATTCGGGGTTTTCG CATCGAAACTGGGGAAATCGAAGCCGTTTTAAGTCAA TATTTCCTATTAGCTGAAAGTGTAGTCGTTGCCAAGG AAGATAATACTGGGGATAAACGCCTCGTGGCTTATTT GGTTCCCGCCTTGCAAAATGAGGCCCTACCAGAGCAA TTAGCCCAATGGCAAAGTGAATACATCAGTGATTGGC AAAGTCTCTATGAAAGAACCTATAGTCAAGGGCAAGA CAGCCTAGCTGATCTCACTTTTAATATCACGGGTTGG AATAGCAGTTATACTCGTCAACCCCTTCCTGCTTCAG AAATGCGAGAGTGGGTCGAAAACACTGTTAGTCGCAT CTTGGCTTTCCAACCAGAACGCGGTTTAGAAATTGGT TGTGGTACAGGTTTGTTACTCTCCAGGGTAGCAAAGC ATTGTCTTGAATATTGGGCAACGGATTATTCCCAAGG GGCGATCCAGTATGTTGAACGGGTTTGCAATGCCGTT GAAGGTTTAGAACAGGTTAAATTACGCTGTCAAATGG CAGATAATTTTGAAGGTATTGCCCTACATCAATTTGA TACCGTCGTCTTAAATTCGATTATTCAGTATTTTCCC AGTGTGGATTATCTGTTACAGGTGCTTGAAGGGGCGA TCAACGTCATTGGCGAGCGAGGTCAGATTTTTGTCGG GGATGTGCGGAGTTTACCCCTATTAGAGCCATATCAT GCGGCTGTGCAATTAGCCCAAGCTTCTGACTCGAAAA CTGTTGAACAATGGCAACAACAGGTGCGTCAAAGTGT AGCAGGTGAAGAAGAACTGGTCATTGATCCCACATTG TTCCTGGCTTTAAAACAACATTTTCCGCAAATTAGCT GGGTAGAAATTCAACCGAAACGGGGTGTGGCTCACAA TGAGTTAACTCAATTTCGCTATGATGTCACTCTCCAT TTAGAGACTATCAATAATCAAGCATTATTGAGCGGCA ATCCAACGGTAATTACCTGGTTAAATTGGCAACTTGA CCAACTGTCTTTAACACAAATTAAAGATAAATTATTA ACAGACAAACCTGAATTGTGGGGAATTCGTGGTATTC CTAATCAGCGAGTTGAAGAGGCTCTAAAAATTTGGGA ATGGGTGGAAAATGCCCCTGATGTTGAAACGGTTGAA CAACTCAAAAAACTTCTCAAACAACAAGTAGATACTG GTATTAATCCTGAACAGGTTTGGCAATTAGCTGAGTC TCTCGGTTACACCGCTCACCTTAGTTGGTGGGAAAGT AGTCAAGACGGTTCCTTTGATGTCATTTTTCAGCGGA ATTCAGAAGCGGAGGACTCAAAAAAATTAACCCTTTC AAAACTTGCTTTCTGGGATGAAAAACCCTTTAAAATA AAGCCCTGGAGTGACTATACTAACAACCCTCTGCGCG GTAAGTTAGTCCAAAAATTAATTCCTAAAGTACGAGA ATTTCTGCAAGAAAAACTACCCAGTTATATGGTTCCC CAGGCGTTTGTGCTGCTTGATTCCCTTCCTTTGACCC CCAATGGTAAGGTGGATCGTAAGGCGTTACCTTCTCC TGATGCGGCGACTCGTGATTTAGCGAACAGTTTTGTC TTACCCCGCAATCCGATTGAAGCTCAACTGACTCAAA TTTGGAGTGAAGTTTTGGGACTGGAACGCATTGGCGT TAAGGACAACTTTTTTGAATTGGGAGGACATTCTCTT TTGGCTACCCAGGTTTTATCAAGAATTAATTCAGCCT TTGGACTTGATCTTTCTGTGCAAATTATGTTTGAATC ACCAACGATCGCGGGCATTGCGGGTTATATTCAAGCG GTAGATTGGGTCGCCCAGGATCAAGCCGATAGCTCGT TAAATCATGAAAATACTGAGGTAGTGGAGTTCTAAGT TATGACGAAAAAGATTGTTGAATTTGTCTGTTATCTA CGGGATTTAGGCATTACTTTAGAAGCTGATGAAAACC GCTTACGCTGTCAGGCTCCCGAAGGAATTTTGACCCC AGCACTCCGTCAAGAAATTGGCGATCACAAACTGGAA TTATTACAATTTTTACAATGGGTCAAACAGTCTAAAA GTACCGCTCATTTGCCTATTAAACCTGTCGCTAGAGA CGGTCATTTACCCCTGTCTTTTGCTCAACAACGTTTA TGGTTTTTACATTATCTTTCCCCTGATAGTCGTTCCT ACAATACCCTGGAAATATTGCAAATTGATGGGAATCT CAATCTGACTGTGCTAGAGCAGAGTTTGGGGGAATTA ATTAACCGCCATGAAATTTTTAGAACAACATTCCCCA CTGTTTCAGGGGAACCGATTCAGAAAATTGCACTTCC TAGTCGTTTTCAGTTAAAAGTTGATAATTATCAAGAT TTAGACGAAAATGAACAATCAGCTAAAATTCAACAAG TAGCAGAATTGGAAGCAGGACAAGCTTTTGATTTAAC GGTGGGGCCACTGATTCAGTTTAAGCTATTGCAATTG AGTCCCCAGAAGTCGGTGCTGCTGTTGAAAATGCACC ATATTATCTATGATGGCTGGTCTTTTGGGATTCTGAT TCGGGAATTATCGGCTCTATACGAAGCATTTTTAAAG AACTTAGCCAATCCTCTCCCTGCGTTGTCTATTCAGT ATGCAGATTTTGCGGTTTGGCAACGTCAATATCTCTC AGGTGAGGTCTTAGATAAACAACTCAATTATTGGCAA GAACAGTTAGCAACAGTCTCTCCTGTTCTTACTTTAC CAACGGATAGACCCCGTCCGGCGATACAAACTTTTCA GGGAGGAGTTGAGCGTTTTCAACTGGATCAAAATGTC ACTCAAGGTCTTAAAAAGTTAGGTCAAGATCAGGTTG CAACCCTGTTTATGACGTTGTTGGCCGGTTTCGGCGT TTTGCTATCTCGTTATAGTGGTCAATCTGATCTGATG GTGGGTTCTCCGATCGCTAATCGTAATCAAGCAGCGA TCGAACCTTTAATTGGCTTTTTTGCTAACACTTTGGC TTTAAGAATTAATTTATCAGAAAATCCCAGTTTTTTA GAATTATTAGAACAAGTTAAACAGACAACTTTAGAGG GTTATGCTCACCAAGACCTACCCTTTGAGATGTTAGT AGAAAAGCTACAACTTGACCGTGATTTGAGCAGAAAT CCTTTAGTACAAGTCATGTTTGCGCTACAAAATACCT CTCAAGATACTTGGAATCTTTCGGGTTTAAGTATTGA AAGTTTATCTTTATCAGTGGAAGAAACTGTCAGATTT GATCTAGAAGTAAACTGCTGGCAAAATTCAGAAGGTT TAGCAATAGATTGGATTTACAGCAGAGATTTATTTGA CACTGCAACAATTGCAAGAATGGGAGAACATTTTCAA AATTTAGTTCAGGCAATCATACTCAATCCAAAAGCTA CAGTTAAAGAACTTCCTTTATTAACACCCAAGGAACG TGAGCAATTATTAATATCTTGGAATAATAGCAAGACT GATTATCCTCAAGAGCAGTGTATTTATCAATTATTTG AAGCACAAGTTGAACGGACTCCAAAGGCGATCGCAGT GGTATTTGAGGAGCAATCATTAACATACACTGAATTA AACCATCGCGCTAATCAGTTAGCCCATTATTTACAAA CTTTAGGCGTGGGAGCAGAAGTCTTAGTCGGTATTTC CCTAGAACGTTCTTTAGAGATGATTATCGGCTTATTA GGGATTCTCAAGGTAGGTGGTGCTTATCTTCCTCTTG ATCCAGACTATCCCACTGAGCGTCTTCAGTTGATGTT AGAAGACAGTCAAGTTCCTTTTTTGATTACCCACAGT TCTTTATTAGCAAAATTGCCTCCCTCTCAAGCAACTC TGATTTGTTTAGATCATATCCAAGAGCAGATTTCTCA ATATTCTCCAGATAATCTTCAATGTCAGTTAACTCCT GCCAATTTAGCTAACGTTATTTATACCTCTGGCTCTA CGGGTAAGCCTAAAGGGGTGATGGTTGAACATAAAGG TTTAGTTAACTTAGCTCTTGCTCAAATTCAATCTTTT GCAGTCAACCATAACAGTCGTGTGCTGCAATTTGCTT CTTTTAGTTTTGATGCTTGTATTTCAGAAATTTTGAT GACCTTTGGTTCTGGAGCGACGCTTTATCTTGCACAA AAAGATGCTTTATTGCCAGGTCAGCCATTAATTGAAC GGTTAGTAAAGAATGGAATTACTCATGTGACTTTGCC GCCTTCAGCTTTAGTGGTTTTACCCCAGGAACCGTTA CGCAACTTAGAAACCTTAATTGTGGCGGGTGAGGCTT GTTCTCTTGATTTAGTGAAACAATGGTCAATCGATAG AAACTTTTTCAATGCCTATGGGCCAACGGAAGCGAGT GTTTGTGCCACTATTGGACAATGTTATCAAGATGATT TAAAGGTGACGATTGGTAAGGCGATCGCCAATGTCCA AATTTATATTTTAGATGCCTTTTTACAGCCGGTGCCG GTGGGAGTGTCAGGAGAGTTATACATTGGTGGAGTTG GGGTGGCAAGGGGCTATTTAAATCGTCCTGAATTAAC CCAAGAAAAATTTATTGCTAATCCTTTTAGTAACGAC CCAGATTCTCGGCTCTATAAAACTGGCGACTTAGCGC GTTATTTACCCGATGGTAATATTGAATATTTAGGACG CATTGACAATCAGGTAAAAATTCGCGGTTTTCGCATT GAGTTAGGAGAAATTGAAGCGGTTCTGAGTCAATGTC CCGATGTGCAAAATACGGCGGTGATTGTCCGCGAAGA TACTCCTGGCGATAAGCGCTTAGTTGCCTATGTGGTT CTTACTTCTGACTCCCAGATAACTACTAGCGAACTGC GTCAATTTTTGGCGAATCAATTACCCGCCTATCTTGT TCCTAATACCTTTGTTATTTTAGATGATTTGCCCCTA ACCCCCAGTGGCAAATGCGATCGCCGTTCCTTACCTA TACCCGAAACACAAGCGTTATCAAATGACTATATTGC CCCTAAATCTCCCACTGAAGAAATTCTGGCTCAAATA TGGGGGCAAGTTCTCAAGATAGAAAGAGTCAGCAGAG AAGATAATTTCTTTGAATTGGGGGGGCATTCCCTTTT AGCTACCCAGGTAATGTCCCGTCTGCGTGAAACTTTT CAAGTCGAATTACCTTTGCGTAGTCTCTTTACCGCTC CCACTATTGCTGAATTGGCCCTAACAATTGAGCAATC TCAGCAAACCATTGCTGCTCCCCCCATCCTAACCAGA AACGACAGTGCTAACCTCCCGTTATCTTTTGCTCAAC AACGTTTATGGTTTCTGGATCAATTAGAACCTAACAG CGCCTTTTATCATGTAGGGGGAGCCGTAAGACTAGAA GGAACATTAAATATTACTGCCTTAGAGCAAAGCTTAA AAGAAATTATTAATCGTCATGAAGCTTTACGCACAAA TTTTATAACGATTGATGGTCAAGCCACTCAAATTATT CACCCTACTATTAATTGGCGATTGTCTGTTGTTGATT GTCAAAATTTAACCGACACTCAATCTCTGGAAATTGC GGAAGCTGAAAAGCCCTTTAATCTTGCTCAAGATTGC TTATTTCGTGCTACTTTATTCGTGCGATCACCGCTAG AATATCATCTACTCGTGACCATGCACCATATTGTTAG CGATGGCTGGTCAATTGGAGTATTTTTTCAAGAACTA ACTCATCTTTACGCTGTCTATAATCAGGGTTTACCCT CATCTTTAACGCCTATTAAAATACAATATGCTGATTT TGCGGTCTGGCAACGGAATTGGTTACAAGGTGAAATT TTAAGTAATCAATTGAATTATTGGCGCGAACAATTAG CAAATGCTCCTGCTTTTTTACCTTTACCGACAGATAG ACCTAGGCCCGCAATCCAAACTTTTATTGGTTCTCAT CAAGAATTTAAACTTTCTCAGCCATTAAGCCAAAAAT TGAATCAACTAAGTCAGAAGCATGGAGTGACTTTATT TATGACTCTCCTGGCTGCTTTTGCTACCTTACTTTAC CGTTATACAGGACAAGCAGATATTTTAGTTGGTTCTC CTATTGCTAACCGTAATCGTAAGGAAATTGAGGGATT AATCGGCTTTTTTGTTAATACATTAGTTCTGAGATTG AGTTTAGATAATGATTTAAGTTTTCAAAATTTGCTAA ACCATGTTAGAGAGGTTTCTTTAGCAGCCTACGCCCA TCAAGATTTACCTTTTGAAATGTTAGTAGAAGCACTA CACCCTCAACGAGATCTCAGTCATACCCCTTTATTTC AGGTAATGTTTGTTTTGCAAAATACACCAGTGGCTGA TCTAGAACTTAAAAATGTAAAGGTTTGTCCTCTACCG ATGGAAAATAAGACTGCTAAATTTGATTTAACCTTAT CAATGGAGAATCTAGAGGAAGGATTGATTGGGGTTTG GGAATATAACACCGATCTATTTAATGGCTCAACCATT GAGCGAATGAGTGGACATTTTGTCACTTTGTTAGAAG ATATTGTTGCCGCTCCAACGAAGTCAGTTTTACGGTT GTCTTTGCTGACGCAAGAGGAAAAACTGCAATTATTG ATTAAAAATCAGGGTGTTCAAGTTGATTATTCTCAAG AGCAGTGCATCCATCAATTATTTGAAGCGCAAGTTGA ACGGACTCCCGATGCGATTGCGGTGGTATTTGAGGAG CAATCATTAACCTATGCTGAATTAAATCATCAAGCTA ATCAGTTAGTCCATTACTTACAAACTTTAGGAATTGG GCCAGAGGTCTTAGTCGCTATTTCAGTAGAACGTTCT TTAGAAATGATTATCGGCTTATTAGCCATTCTCAAGG CGTGTGGTGCTTATCTCCCTCTTGCTCCTGACTATCC CACTGAGCGTCTTCAGTTCATGTTAGAAGATAGTCAA GCTTCTTTTTTGATTACCCACAGTTCTTTATTAGAAA AATTGCCTTCTTCTCAAGCGACTCTAATTTGTTTAGA TCACATCCAAGAGCAGATTTCTCAATATTCTCCCGAT AATCTTCAAAGTGAGTTAACTCCTTCCAATTTGGCTA ACGTTATTTACACCTCTGGCTCTACGGGTAAGCCTAA AGGGGTGATGGTTGAACATCGGGGCTTAGTTAACTTA GCGAGTTCTCAAATTCAATCTTTTGCAGTCAAAAATA ACAGTCGTGTACTGCAATTTGCTTCCTTTAGTTTTGA TGCTTGTATTTCAGAAATTTTGATGACCTTTGGTTCT GGAGCGACTCTTTATCTTGCTCAAAAAAATGATTTAT TGCCAGGTCAGCCATTAATGGAAAGGTTAGAAAAGAA TAAAATTACCCATGTTACTTTACCCCCTTCAGCTTTA GCTGTTTTACCAAAAAAACCGTTACCCAACTTACAAA CTTTAATTGTGGCGGGTGAGGCTTGTCCTCTGGATTT AGTCAAACAATGGTCAGTCGGTAGAAACTTTTTCAAT GCCTATGGCCCGACAGAAACGAGTGTTTGTGCCACGA TTGGACAATGTTATCAAGATGATTTAAAGGTCACGAT TGGTAAGGCGATCGCTAATGTCCAAATTTATATTTTG GATGCCTTTTTACAACCAGTACCCATCGGAGTACCAG GGGAATTATACATTGGTGGAGTCGGAGTTGCGAGGGG TTATCTAAATCGTCCTGAATTAACGGCGGAAAGATTT ATTCCTAATCCTTTTGATCCCCCCCTAACCCCCCTTA AAAAGGGGGGAGATAAGAGCTATGAAACTTTTAAAAA GGGGGAAGAGCAACCATCAAAACTCTATAAAACGGGA GATTTAGCTCGTTATTTACCCGATGGCAATATTGAAT ATTTAGGACGCATTGACAATCAGGTAAAAATTCGCGG TTTTCGCATTGAGTTAGGAGAAATTGAAGCGGTTCTG AGTCAATGTCCCGATGTGCAAAATACGGCGGTGATTG TCCGTGAAGATACTCCTGGCGATAAACGTTTAGTTGC CTATGTGGTTCTTACTTCTGACTCCCAGATAACTACT AGCGAACTGCGTCAATTCTTGGCTAATCAATTACCTG CCTATCTCGTTCCCAATACCTTTGTTATTTTAGATGA TTTGCCCCTAACCCCCAATGGTAAATGCGATCGCCGT TCCTTACCGCTTCCTGATGATCAGACCAGAAAAAATA TTCCTAAAATTGGCCCGCGTAATTTAGTGGAATTACA ATTAGCTCAAATCTGGTCAGAGATTTTAGGCATTAAT AATATTGGTATTCAGGAAAACTTCTTTGAATTAGGCG GTCATTCTTTATTAGCAGTCAGTCTGATCAATCGTAT TGAACAAAAGTTAGATAAACGTTTACCATTAACCAGT CTTTTTCAAAATGGAACCATAGCAAGTCTAGCTCAAT TACTAGCGCAAGAAACAACTCAGCCAGCCTCTTCACC GTTGATTGCTATCCAGTCTCAAGGTGATAAAACTCCA TTTTTTGCTGTTCATCCCATTGGTGGTAATGTGCTAT GTTATGCCGATTTAGCTCGTAATTTAGGAACGAAACA GCCGTTTTATGGATTACAATCATTAGGGCTAAGTGAA TTAGAAAAAACTGTAGCCTCTATTGAAGAAATGGCGA TGATTTATATTGAAGCAATACAAACTGTTCAAGCCTC TGGTCCCTACTATTTAGGAGGTTGGTCAATGGGAGGA GTGATAGCTTTTGAAATCGCCCAACAATTATTGACCC AAGGTCAAGAAGTTGCTTTACTGGCTTTAATAGATAG TTATTCTCCCAGTTTACTTAATTCAGTTAATAGGGAG AAAAATTCTGCTAATTCCCTGACAGAAGAATTTAATG AAGATATCAATATTGCCTATTCTTTCATCAGAGACTT AGCAAGTATATTTAATCAAGAAATCTCTTTCTCTGGG AGTGAACTTGCTCATTTTACATCAGACGAATTACTAG ACAAGTTTATTACTTGGAGTCAAGAGACGAATCTTTT GCCGTCAGATTTTGGGAAGCAGCAGGTTAAAACCTGG TTTAAAGTTTTCCAGATTAATCACCAAGCTTTGAGCA GCTATTCTCCCAAGACGTATCTGGGTAGAAGTGTTTT CTTAGGAGCGGAAGACAGTTCTATTAAAAATCCTGGT TGGCATCAAGTAATCAATGACTTGCAATCTCAATGGA TTAGCGGCGATCACTACGGTTTAATTAAAAATCCAGT CCTCGCTGAAAAACTCAATAGCTACCTAGCCTAAAAC TTTCAAAAAGCCTGATTATTGTTTAAAATGAATGATC GTTCACCGGTCAGAGGACAAGTATGACAACCCAAACA GCTTCTAGTGCCAATGCCCTTGCTTCCTTTAACCAAT TTTTAAGGGATGTAAAGGCGATCGCCCAACCCTATTG GTATCCCACTGTATCAAATAAAAGAAGCTTTTCTGAG GTTATTCGTTCCTGGGGAATGCTATCACTGCTTATCT TTTTGATTGTGGGATTAGTCGCCGTCACGGCTTTTAA TAGTTTTGTTAATCGTCGTTTAATTGATGTCATTATT CAAGAAAAAGATGCGTCTCAATTTGCCAGTACATTAA CTGTCTATGCGATCGGATTAATCTGTGTAACGCTGCT GGCAGGGTTCACTAAAGATATTCGCAAAAAAATTGCC CTAGATTGGTATCAATGGTTAAACACCCAGATTGTAG AGAAATATTTTAGTAATCGTGCCTATTATAAAATTAA CTTTCAATCTGACATTGATAACCCCGATCAACGTCTA GCCCAGGAAATTGAACCGATCGCCACAAACGCCATTA GTTTCTCGGCCACTTTTTTGGAAAAAAGTTTGGAAAT GCTAACTTTTTTAGTGGTAGTTTGGTCAATTTCTCGA CAGATTGCTATTCCGCTAATGTTTTACACGATTATCG GTAATTTTATTGCCGCCTATCTAAATCAAGAATTAAG CAAGATCAATCAGGCACAACTGCAATCAAAAGCAGAT TATAACTATGCCTTAACCCATGTTCGGACTCATGCGG AATCTATTGCTTTTTTTCGGGGAGAAAAAGAGGAACA AAATATTATTCAGCGACGTTTTCAGGAAGTTATCAAT GATACGAAAAATAAAATTAACTGGGAAAAAGGGAATG AAATTTTTAGTCGGGGCTATCGTTCCGTCATTCAGTT TTTTCCTTTTTTAGTCCTTGGCCCTTTGTATATTAAA GGAGAAATTGATTATGGACAAGTTGAGCAAGCTTCAT TAGCTAGTTTTATGTTTGCATCGGCCCTGGGAGAATT AATTACAGAATTTGGTACTTCAGGACGTTTTTCTAGT TATGTAGAACGTTTAAATGAATTTTCTAATGCCTTAG AAACTGTGACTAAACAAGCCGAGAATGTCAGCACAAT TACAACCATAGAAGAAAATCATTTTGCCTTTGAACAC GTCACCCTAGAAACCCCTGACTATGAAAAGGTGATTG TTGAGGATTTATCTCTTACTGTTCAAAAAGGTGAAGG ATTATTGATTGTCGGGCCCAGTGGTCGAGGTAAAAGT TCTTTATTAAGGGCGATCGCCGGTTTATGGAATGCTG GCACTGGGCGTTTAGTGCGTCCTCCCCTAGAAGAAAT TCTCTTTTTGCCCCAACGTCCCTACATTATTTTGGGA ACCTTACGCGAACAATTGCTGTATCCTCTAACCAATA GTGAGATGAGCAATACCGAACTTCAAGCAGTATTACA ACAAGTCAATTTGCAAAATGTGCTAAATCGGGTGGAT GACTTTGACTCCGAAAAACCCTGGGAAAACATTCTCT CCCTCGGTGAACAACAACGCCTAGCCTTTGCTCGATT GTTAGTGAATTCTCCGAGTTTTACCATTTTAGATGAG GCGACCAGTGCCTTAGATTTAACAAATGAGGGGATTT TATACGAGCAATTACAAACTCGCAAGACAACCTTTAT TAGTGTGGGTCATCGAGAAAGTTTGTTTAATTACCAT CAATGGGTTTTAGAACTTTCTGCTGACTCTAGTTGGG AACTCTTAAGCGTTCAAGATTATCGCCTTAAAAAAGC GGGAGAAATGTTTACTAATGCTTCGAGTAACAATTCC ATAACACCCGATATTACTATCGATAATGGATCAGAAC CAGAAATAGTCTATTCTCTTGAAGGATTTTCCCATCA GGAAATGAAACTATTAACAGACCTATCACTCTCTAGC ATTCGGAGTAAAGCCAGTCGAGGGAAGGTGATTACAG CCAAGGATGGTTTTACCTACCTTTATGACAAAAATCC TCAGATATTAAAGTGGCTCAGAACTTAA 

1. Nucleic acid encoding a microginin synthetase enzyme complex with the following activities: a) adenylation domain (A*) wherein, the adenylation domain comprises a peptide sequence according to SEQ ID NO. 1 b) acyl carrier protein (ACP) c) elongation module (EM) of polyketide synthases (PKS) comprising the following activities: i. ketoacylsynthase (KS) ii. acyl transferase (AT) iii. acyl carrier protein (ACP 2) d) aminotransferase (AMT) e) three to five elongation modules (EM) of non-ribosomal peptide synthetases (NRPS) comprising the following activities: i. condensation domain (C) ii. adenylation domain (A) iii. thiolation domain (T) f) thioesterase (TE) or, a derivative of the nucleic acid molecule having the function of a microginin synthetase enzyme complex;
 2. Nucleic acid according to claim 1, additionally and optionally comprising sequences encoding the following activities or domains: a) a monooxygenase (MO) b) an integrated N-methyltransferase domain (MT) within one or more elongation modules (EM) of NRPS; c) a non-integrated N-methyltrasferase (MT), d) a modifying activity (MA) wherein, said MA is selected from the group comprising the following activities: halogenase, sulfatase, glycosylase, racemase, O-methyltransferase and C-methyltransferase e) two or more peptide repeat spacer sequences (SP) consisting of one or more repeats of being either glycine rich or proline and leucine rich, located adjacently upstream and downstream of the MO and/or another MA.
 3. Nucleic acid according to claim 1 or 2 wherein, the nucleic acid may comprise nucleic acid sequences encoding protein sequences as follows: a. adenylation domain (A*) according to SEQ ID NO. 1 b. acyl carrier protein (ACP) according to SEQ ID NO. 2 c. elongation module of polyketide synthases: i. ketoacylsynthase domain (KS) according to SEQ ID NO. 3 ii. acyl transferase domain (AT) according to SEQ ID NO. 4 iii. acyl carrier protein domain (ACP 2) according to SEQ ID NO. 5 d. aminotransferase (AMT) according to SEQ ID NO. 6 e. elongation modules of non-ribosomal peptide synthetases: i. condensation domain (C) according to SEQ ID NO. 7 ii. adenylation domain (A) according to SEQ ID NO. 8 iii. thiolation domains (T) according to SEQ ID NO. 9 f. elongation modules of non-ribosomal peptide synthetases responsible for the activation and condensation of leucin: i. condensation domain (C 2) according to SEQ ID NO. 10 ii. adenylation domain (A 2) according to SEQ ID NO. 11 iii. thiolation domain (T 2) according to SEQ ID NO. 12 g. elongation modules of non-ribosomal peptide synthetases responsible for the activation and condensation of trosin 2: i. condensation domain (C 3) according to SEQ ID NO. 13 ii. adenylation domain (A 3) according to SEQ ID NO. 14 iii. thiolation domain (T 3) according to SEQ ID NO. 15 h. elongation modules of non-ribosomal peptide synthetases responsible for the activation and condensation of trosin 2: i. condensation domain (C 4) according to SEQ ID NO. 16 ii. adenylation domain (A 4) according to SEQ ID NO. 17 iii. thiolation domain (T 4) according to SEQ ID NO. 18 i. thioesterase (TE) according to SEQ ID NO. 19 j.) monooxygenase (MO) according to SEQ ID NO. 20 k.) two or more peptide repeat spacer sequences (SP1/SP2) according to SEQ ID NO. 21 and 22 l.) an integrated N-methyltransferase domain (MT) within the elongation module (EM) of the NRPS responsible for the activation and condensation of leucin according to SEQ ID 23 and m.) a non-integrated N-methyltransferase (MT 2) according to SEQ ID NO.
 24. 4. Nucleic acid according to claim 1 may contain nucleic acids selected from the group comprising: a) an adenylation domain (A*) according to SEQ ID NO. 25, b) acyl carrier protein (ACP) according to SEQ ID NO. 26, c) elongation module of polyketide synthases encoding for the condensation of acetate: i. ketoacylsynthase domain (KS) according to SEQ ID NO. 27 ii. acyl transferase domain (AT) according to SEQ ID NO. 28 iii. acyl carrier protein domain (ACP 2) according to SEQ ID NO. 29 d) aminotransferase (AMT) according to SEQ ID NO. 30, e) elongation modules of non-ribosomal peptide synthetases encoding for the activation and condensation of alanin: i. condensation domain (C) according to SEQ ID NO. 31 ii. adenylation domain (A) according to SEQ ID NO. 32 iii. thiolation domain (T) according to SEQ ID NO. 33 f) elongation modules of non-ribosomal peptide synthetases encoding for the activation and condensation of leucin: i. condensation domain (C 2) according to SEQ ID NO. 34 ii. adenylation domain (A 2) according to SEQ ID NO. 35 iii. thiolation domain (T 2) according to SEQ ID NO. 36 g) elongation modules of non-ribosomal peptide synthetases encoding for the activation and condensation of tyrosin 1: i. condensation domains (C 3) according to SEQ ID NO. 37 ii. adenylation domains (A 3) according to SEQ ID NO. 38 iii. thiolation domains (T 3) according to SEQ ID NO. 39 h) elongafion modules of non-ribosomal peptide synthetases encoding for the activation and condensation of trosin 2: i. condensation domains (C 4) according to SEQ ID NO. 40 ii. adenylation domains (A 4) according to SEQ ID NO. 41 iii. thiolation domains (T 4) according to SEQ ID NO. 42 i) thioesterase (TE) according to SEQ ID NO. 43 j) monooxygenase (MO) according to SEQ ID NO. 44 k) two or more peptide repeat spacer sequences (SP1/2) according to SEQ ID NO. 45 and
 46. l.) an integrated N-methyltransferase domain (MT) within the elongation module (EM) of the NRPS encoding for the activation and condensation of leucin according to SEQ ID 47 and m.) a non-integrated N-methyltrasferase (MT 2) according to SEQ ID NO.
 48. 5. Nucleic acid according to claim 1 wherein, the sequence parts of the nucleic acid encoding the microginin synthetase enzyme complex are arranged in an upstream to downstream manner as depicted in FIG.
 1. 6. A vector comprising the nucleic acid of claim
 1. 7. A microorganism transformed with a nucleic acid according to claim
 1. 8. A microorganism according to claim 7 wherein, the vector is able to replicate autonomously.
 9. A method of producing a microginin, comprising culturing a cell under conditions under which the cell will produce microginin, wherein said cell comprises a nucleic acid encoding a recombinant microginin, according to claim 1, and wherein said cell does not produce the microginin in the absence of said nucleic acid.
 10. Nucleic acids according selected from the group of a) nucleic acid according to SEQ ID NO. 49 (Primer A), b) nucleic acid according to SEQ ID NO. 50 (Primer B), c) nucleic acid according to SEQ ID NO. 51 (Primer C), d) nucleic acid according to SEQ ID NO. 52 (Primer D), e) nucleic acid according to SEQ ID NO. 53 (Primer E), f) nucleic acid according to SEQ ID NO. 54 (Primer F), g) nucleic acid according to SEQ ID NO. 55 (Primer G), h) nucleic acid according to SEQ ID NO. 56 (Primer H), i) nucleic acid according to SEQ ID NO. 57 (Primer I) and j) nucleic acid according to SEQ ID NO. 58 (Primer J).
 11. Method for detecting a microginin synthetase gene cluster in a sample wherein, one or more of the nucleic acids according to claim 10 are, applied in an amplification and/or a hybridization reaction.
 12. Method according to claim 11 wherein primers D and F or H and J or E and I or E and A are added to a PCR reaction mixture comprising a sample and wherein presence of an amplification product represents presence of microginin synthetase gene cluster and absence of an amplification product represents absence of a microginin synthetase gene cluster.
 13. Antibody against peptide according to SEQ ID NO.
 1. (A*)
 14. Nucleic acid encoding a peptide repeat spacer sequence (SP) wherein, a) the peptide sequence comprises at least 4 consecutive glycin amino acids or, b) at least 4 proline and/or leucin amino acids, c) a single repeat unit (SRU) within the SP is between 4 and 18 amino acids in length and, d) the SP comprises between X and Y SRUs.
 15. Nucleic acid according to claim 14, encoding a peptide SRU with a sequence as shown in SEQ ID NO. 20 or SEQ ID NO.
 21. 16. Nucleic acid according to claim 15, with a sequence as laid down in SEQ ID NO. 43 or SEQ ID NO.
 44. 17. Method of producing recombinant microginin variants comprising, a) modifying the nucleic acid according to claim 1 in vitro or in vivo, b) growing a recombinant cell comprising said recombinantly modified nucleic acid under conditions which lead to synthesis of a microginin and, c) recovering the synthesized microginin.
 18. Method according to claim 14 wherein, said modifying of said nucleic acid maybe an action selected from the group of one or more of the following actions: a) inactivation of one or more of the MT present, b) substitution of one or more of the MTs present with a halogenase, a sulfatase, a glycosylase, a racemase, an O-methyltransferase or a C-methyltransferase, c) inactivation of the MO, d) substitution of the MO with a halogenase, a sulfatase, a glycosylase, a racemase, an O-methyltransferase or a C-methyltransferase, e) inactivation of the AMT, f) substitution of the AMT with a halogenase, a sulfatase, a glycosylase, a racemase, an O-methyltransferase or a C-methyltransferase, g) inactivation of the PKS module h) substitution of the entire PKS module with an alternative PKS module and/or substitution of a one or more of the domains (KS, AT, ACP) therein, i) inactivation of the A* domain, j) substitution of the A* domain with alternative A domains, k) inactivation of one or more of the NRPS modules and l) substitution of one or more of the NRPS modules with alternative NRPS modules and/or substitution of one or more of the domains (C, A, T) therein.
 19. Method according to claim 17 wherein, said alternative modules or domains which are used for substitution of the original module or domain, additionally may comprise one or more SP nucleic acids with a sequence as laid down in SEQ ID NO. 43 or SEQ ID NO. 44 located adjacently upstream of the module or domain used for substitution and one or more SP nucleic acids with a sequence as laid down in SEQ ID NO. 43 or SEQ ID NO. 44 located adjacently downstream of the module or domain used for substitution.
 20. A microorganism transformed with a vector according to claim
 6. 